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https://zephyrnet.com/NCT03797807
2019-03-20
https://zephyrnet.com/?p=NCT03797807
NCT03797807https://www.clinicaltrials.gov/study/NCT03797807?tab=tableVandana Luthra, Dr.BHNT.Clinicaloralresearchcentre@nhs.net02078826348To compare the efficacy of a modified minimally-invasive non-surgical periodontal therapy (MINST) approach with a surgical approach (M-MIST) in determining bone and clinical attachment changes in intrabony defects
<![CDATA[
Studies
Study First Submitted Date | 2018-12-19 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2023-05-26 |
Start Month Year | March 20, 2019 |
Primary Completion Month Year | April 30, 2025 |
Verification Month Year | May 2023 |
Verification Date | 2023-05-31 |
Last Update Posted Date | 2023-05-26 |
Detailed Descriptions
Sequence: | 20668410 |
Description | Periodontal diseases are inflammatory conditions that affect the supporting apparatus of the teeth, including gingiva and alveolar bone. The bone loss resulting from periodontitis often is irregular and localised, giving onset to 'intrabony' or 'vertical defects' affecting one side of the tooth more than the other and more than on the neighbouring teeth. Periodontal intrabony defects have been associated with a higher risk of further progression and eventually tooth loss.
The treatment of periodontitis involves a non-specific reduction of the bacterial load below the gingival margin. This is achieved by oral hygiene instructions (OHI) and non-surgical periodontal therapy (NSPT), aimed at removing calculus and disrupting the plaque biofilm from the affected root surfaces. Intrabony defects are considered sites requiring therapy, often beyond NSPT. Decades ago, intrabony defects were treated with surgical elimination of the defect achieved by sacrificing the adjacent healthy supportive or non-supportive bone. More recently periodontal regenerative procedures have been advocated for deep intrabony defects, which are considered amenable for guided tissue regeneration. This technique results in regeneration of periodontal attachment measurable histologically and radiographically and measurable clinically. However, this is associated with potential morbidity and high costs due to the use of bone graft and barrier materials and is not always predictable. The more recent introduction of minimally-invasive surgical therapy (MIST), modified-MIST (M-MIST) and single-flap approach suggested that the use of biomaterials may not be so crucial for obtaining periodontal regeneration. Retrospective studies from the investigator's group have shown that minimally invasive non-surgical periodontal treatment of intrabony defects results in clinical improvements (measured as PPD reductions and clinical attachment level-CAL- gain) but also in bone fill of the bony defects, measurable radiographically. The extent of the radiographic resolution of the defect was positively associated with initial defect depth and use of adjunctive antibiotics, while smoking seemed to negatively influence this outcome. A non-surgical minimally-invasive treatment protocol, named MINST, has been proposed along these principles. A more recent retrospective analysis has revealed a reduction in bony defect of nearly 3 mm for cases treated with minimally-invasive non-surgical therapy. The effect of MINST may be mediated by improved blood flow and stable blood clot in the intrabony defect. However, very few studies have been published on MINST and no data are available on the comparison between MINST and MIST. This is a parallel group, single centre, examiner-blind, non-inferiority randomized controlled trial to compare the effect of a modified minimally-invasive non-surgical therapy (MINST) approach to minimally invasive surgical treatment (MIST) in the healing of periodontal intrabony defects in 66 patients with periodontitis . |
Facilities
Sequence: | 199508244 |
Status | Recruiting |
Name | Barts and The London Dental Hospital |
City | London |
Zip | E1 2AD |
Country | United Kingdom |
Facility Contacts
Sequence: | 28041986 | Sequence: | 28041987 |
Facility Id | 199508244 | Facility Id | 199508244 |
Contact Type | primary | Contact Type | backup |
Name | Rinat Ezra, PhD | Name | Simona Salomone, PhD |
BHNT.Clinicaloralresearchcentre@nhs.net | BHNT.Clinicaloralresearchcentre@nhs.net | ||
Phone | 0207 882 6348 | Phone | 0207 882 6064 |
Phone Extension | 6348 | Phone Extension | 6064 |
Conditions
Sequence: | 52032178 |
Name | Periodontitis |
Downcase Name | periodontitis |
Id Information
Sequence: | 40049393 |
Id Source | org_study_id |
Id Value | 18/LO/1956 |
Countries
Sequence: | 42447076 |
Name | United Kingdom |
Removed | False |
Design Groups
Sequence: | 55440100 | Sequence: | 55440101 | Sequence: | 55440102 | Sequence: | 55440103 |
Group Type | Experimental | Group Type | Active Comparator | Group Type | Active Comparator | Group Type | Active Comparator |
Title | MINST | Title | MIST | Title | GTI + MINST | Title | GTI + MIST |
Description | Minimally invasive non surgical treatment | Description | Minimally invasive surgical treatment | Description | Minimally invasive non surgical treatment + Geometric/Thermal Imaging (GTI subgroup) | Description | Minimally invasive surgical treatment + Geometric/Thermal Imaging (GTI subgroup) |
Interventions
Sequence: | 52344252 | Sequence: | 52344253 | Sequence: | 52344254 |
Intervention Type | Procedure | Intervention Type | Procedure | Intervention Type | Diagnostic Test |
Name | MINST | Name | MIST | Name | GTI subgroup (Geometrical/Thermal Imaging) |
Description | A non-surgical minimally invasive treatment protocol, named MINST, has been proposed for the treatment of periodontal intrabony defects, in order to minimize patient discomfort and maximize the healing potential | Description | A minimally invasive surgical treatment protocol, named MIST, has been proposed for the treatment of periodontal intrabony defects, in order to minimize patient discomfort and maximize the healing potential | Description | Geometrical/Thermal Imaging |
Design Outcomes
Sequence: | 176898043 | Sequence: | 176898044 | Sequence: | 176898045 | Sequence: | 176898046 | Sequence: | 176898047 | Sequence: | 176898048 | Sequence: | 176898049 | Sequence: | 176898050 | Sequence: | 176898051 |
Outcome Type | primary | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other |
Measure | Radiographic whole defect depth change | Measure | Probing Pocket Depth (PPD) change | Measure | Clinical Attachment Level (CAL) gain change | Measure | Markers and growth factors in gingival crevicular fluid (GCF) | Measure | Bacterial detection | Measure | Gingival inflammation and healing | Measure | Self administered OIDP (oral impact on daily performances index) | Measure | Global ratings on health and quality of life with Visual Analogue Scale (VAS) | Measure | Global ratings on health and quality of life with a question "How would you rate the quality of your life" |
Time Frame | 9 months | Time Frame | Up to 15 months | Time Frame | Up to 15 months | Time Frame | Up to 15 months | Time Frame | Up to 15 months | Time Frame | Up to 15 months | Time Frame | Up to 9 months | Time Frame | Up to 9 months | Time Frame | Up to 9 months |
Description | Radiographic whole defect depth change in millimeters at 9 months [considered a surrogate measure evaluating the entire regenerative process including bone, cementum and periodontal ligament | Description | Probing Pocket Depth (PPD) change (in mm) | Description | Clinical Attachment Level (CAL) gain change (in mm) | Description | Levels of inflammatory markers and growth factors in gingival crevicular fluid (GCF). Specifically, markers related with the healing of epithelium, connective tissue, bone and related to inflammatory/host responses will be examined. | Description | Bacterial detection associated with presence of intrabony defects | Description | Gingival inflammation and healing (as measured by geometric/thermal stereophotogrammetry imaging in the 'GTI sub-study') | Description | We will utilize the oral impact on daily performances index (OIDP) to evaluate health and treatment outcomes. The OIDP focuses on the impact that the conditions of the teeth and mouth have on the physical/functional, psychological and social well-being of the person. Particularly, it assesses the impact of oral conditions on basic daily life activities and behaviours (eating, speaking, cleaning teeth, and going out, relaxing, smiling, major work or role, emotional stability, social contact). For each performance, both the frequency and severity of oral impacts are assessed. The overall OIDP score ranges from 0 to 100, with higher scores indicating worse quality of life. | Description | The VAS records the patient's self-rated health on a vertical visual analogue scale, where the endpoints are labelled 'The best health you can imagine' and 'The worst health you can imagine'. | Description | The responses will be scored on a six-point scale as:
Excellent |
Browse Conditions
Sequence: | 192933827 | Sequence: | 192933828 | Sequence: | 192933829 | Sequence: | 192933830 |
Mesh Term | Periodontitis | Mesh Term | Periodontal Diseases | Mesh Term | Mouth Diseases | Mesh Term | Stomatognathic Diseases |
Downcase Mesh Term | periodontitis | Downcase Mesh Term | periodontal diseases | Downcase Mesh Term | mouth diseases | Downcase Mesh Term | stomatognathic diseases |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48189442 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Queen Mary University of London |
Overall Officials
Sequence: | 29204859 |
Role | Principal Investigator |
Name | Luigi Nibali, PhD |
Affiliation | Barts & The London School of Medicine & Dentistry, QMUL |
Central Contacts
Sequence: | 11978642 |
Contact Type | primary |
Name | Vandana Luthra, Dr. |
Phone | 02078826348 |
BHNT.Clinicaloralresearchcentre@nhs.net | |
Role | Contact |
Design Group Interventions
Sequence: | 67963528 | Sequence: | 67963529 | Sequence: | 67963530 | Sequence: | 67963531 | Sequence: | 67963532 | Sequence: | 67963533 |
Design Group Id | 55440102 | Design Group Id | 55440100 | Design Group Id | 55440103 | Design Group Id | 55440101 | Design Group Id | 55440102 | Design Group Id | 55440103 |
Intervention Id | 52344252 | Intervention Id | 52344252 | Intervention Id | 52344253 | Intervention Id | 52344253 | Intervention Id | 52344254 | Intervention Id | 52344254 |
Eligibilities
Sequence: | 30683699 |
Gender | All |
Minimum Age | 25 Years |
Maximum Age | 70 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
Age 25-70 Exclusion Criteria: 1. Smoking (current or in past 5 years) including e-cigarettes/vaping 2. Medical history including diabetes or hepatic or renal disease, or other serious medical conditions or transmittable diseases 3. History of conditions requiring prophylactic antibiotic coverage prior to invasive dental procedures 4. Antiinflammatory or anticoagulant therapy during the month preceding the baseline exam 5. Systemic antibiotic therapy during the 3 months preceding the baseline exam 6. History of alcohol or drug abuse, 7. Self-reported pregnancy or lactation 8. Other severe acute or chronic medical or psychiatric condition or laboratory abnormality that according to the investigator may increase the risk associated with trial participation, 9. Periodontal treatment to the study site within the last 12 months (excluding not-extensive subgingival debridement as judged by the examining clinician). – |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253886571 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2018 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 25 |
Maximum Age Num | 70 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Other Outcomes To Measure | 8 |
Designs
Sequence: | 30430426 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Single |
Outcomes Assessor Masked | True |
Responsible Parties
Sequence: | 28796932 |
Responsible Party Type | Sponsor |
Study References
Sequence: | 51921492 | Sequence: | 51921493 | Sequence: | 51921494 | Sequence: | 51921495 | Sequence: | 51921496 | Sequence: | 51921497 | Sequence: | 51921498 | Sequence: | 51921499 | Sequence: | 51921500 | Sequence: | 51921501 | Sequence: | 51921502 | Sequence: | 51921503 |
Pmid | 11276518 | Pmid | 2066446 | Pmid | 12787211 | Pmid | 6964676 | Pmid | 11276509 | Pmid | 16625546 | Pmid | 19186978 | Pmid | 21303402 | Pmid | 21091528 | Pmid | 21284549 | Pmid | 26257238 | Pmid | 31351492 |
Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | derived |
Citation | Papapanou PN, Tonetti MS. Diagnosis and epidemiology of periodontal osseous lesions. Periodontol 2000. 2000 Feb;22:8-21. doi: 10.1034/j.1600-0757.2000.2220102.x. No abstract available. | Citation | Papapanou PN, Wennstrom JL. The angular bony defect as indicator of further alveolar bone loss. J Clin Periodontol. 1991 May;18(5):317-22. doi: 10.1111/j.1600-051x.1991.tb00435.x. | Citation | Heitz-Mayfield LJ, Trombelli L, Heitz F, Needleman I, Moles D. A systematic review of the effect of surgical debridement vs non-surgical debridement for the treatment of chronic periodontitis. J Clin Periodontol. 2002;29 Suppl 3:92-102; discussion 160-2. doi: 10.1034/j.1600-051x.29.s3.5.x. | Citation | Nyman S, Lindhe J, Karring T, Rylander H. New attachment following surgical treatment of human periodontal disease. J Clin Periodontol. 1982 Jul;9(4):290-6. doi: 10.1111/j.1600-051x.1982.tb02095.x. | Citation | Cortellini P, Tonetti MS. Focus on intrabony defects: guided tissue regeneration. Periodontol 2000. 2000 Feb;22:104-32. doi: 10.1034/j.1600-0757.2000.2220108.x. No abstract available. | Citation | Needleman IG, Worthington HV, Giedrys-Leeper E, Tucker RJ. Guided tissue regeneration for periodontal infra-bony defects. Cochrane Database Syst Rev. 2006 Apr 19;(2):CD001724. doi: 10.1002/14651858.CD001724.pub2. | Citation | Trombelli L, Farina R, Franceschetti G, Calura G. Single-flap approach with buccal access in periodontal reconstructive procedures. J Periodontol. 2009 Feb;80(2):353-60. doi: 10.1902/jop.2009.080420. | Citation | Cortellini P, Tonetti MS. Clinical and radiographic outcomes of the modified minimally invasive surgical technique with and without regenerative materials: a randomized-controlled trial in intra-bony defects. J Clin Periodontol. 2011 Apr;38(4):365-73. doi: 10.1111/j.1600-051X.2011.01705.x. Epub 2011 Feb 8. | Citation | Nibali L, Pometti D, Tu YK, Donos N. Clinical and radiographic outcomes following non-surgical therapy of periodontal infrabony defects: a retrospective study. J Clin Periodontol. 2011 Jan;38(1):50-7. doi: 10.1111/j.1600-051X.2010.01648.x. Epub 2010 Nov 22. | Citation | Ribeiro FV, Casarin RC, Palma MA, Junior FH, Sallum EA, Casati MZ. Clinical and patient-centered outcomes after minimally invasive non-surgical or surgical approaches for the treatment of intrabony defects: a randomized clinical trial. J Periodontol. 2011 Sep;82(9):1256-66. doi: 10.1902/jop.2011.100680. Epub 2011 Feb 2. | Citation | Nibali L, Pometti D, Chen TT, Tu YK. Minimally invasive non-surgical approach for the treatment of periodontal intrabony defects: a retrospective analysis. J Clin Periodontol. 2015 Sep;42(9):853-859. doi: 10.1111/jcpe.12443. Epub 2015 Sep 29. | Citation | Nibali L, Koidou V, Salomone S, Hamborg T, Allaker R, Ezra R, Zou L, Tsakos G, Gkranias N, Donos N. Minimally invasive non-surgical vs. surgical approach for periodontal intrabony defects: a randomised controlled trial. Trials. 2019 Jul 27;20(1):461. doi: 10.1186/s13063-019-3544-8. |
]]>
https://zephyrnet.com/NCT03797794
2019-01-31
https://zephyrnet.com/?p=NCT03797794
NCT03797794https://www.clinicaltrials.gov/study/NCT03797794?tab=tableHuib Kerstjensh.a.m.kerstjens@umcg.nlNAThe effect of PESF (Pulsating Electrostatic Field) on the oxygen saturation, quality of life and the exercise capacity will be studied in a randomized, dubbel blind, placebo-controlled parallel design with 32 COPD patients GOLD III and IV with a oxygen saturation below or equal to 90%.
The patients will be treated with three 30-minute PESF- or placebo-sessions distributed over 5 days.
Directly before the first session, oxygen saturation, quality of life (CCQuestionnaire), exercise capacity (6-MWT and grip strength) and phase angle (BIA) will be measured and compared to the results directly after the third session. Oxygen saturation is also monitored during 24 hours after each session.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-10 |
Start Month Year | January 2019 |
Primary Completion Month Year | November 1, 2019 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-10 |
Facilities
Sequence: | 199965117 |
Status | Recruiting |
Name | Tjongerschans |
City | Heerenveen |
State | Friesland |
Zip | 8441 PW |
Country | Netherlands |
Facility Contacts
Sequence: | 28086663 |
Facility Id | 199965117 |
Contact Type | primary |
Name | Jaap Westbroek |
j.westbroek@tjongerschans.nl | |
Phone | 0513-685227 |
Conditions
Sequence: | 52139061 |
Name | COPD |
Downcase Name | copd |
Id Information
Sequence: | 40135104 |
Id Source | org_study_id |
Id Value | PESF and COPD |
Countries
Sequence: | 42542719 |
Name | Netherlands |
Removed | False |
Design Groups
Sequence: | 55559415 | Sequence: | 55559416 |
Group Type | Experimental | Group Type | Sham Comparator |
Title | PESF-treatment | Title | Placebo-treatment |
Description | The group undergoing the pulsating electrostatic field intervention | Description | The group undergoing the SHAM Pulsating Electrostatic Field |
Interventions
Sequence: | 52454970 | Sequence: | 52454971 |
Intervention Type | Device | Intervention Type | Device |
Name | Pulsating Electrostatic Field | Name | SHAM Pulsating Electrostatic Field |
Description | A pulsating electrostatic field is generated by the New Health 9000 (Akern). During the session the patients sits on a chair which contains the apparatus for 30 minutes. | Description | The same apparatus which produces the pulsating electrostatic field contains a 'sham-inlet'. This inlet will be used as placebo. |
Design Outcomes
Sequence: | 177264038 | Sequence: | 177264039 | Sequence: | 177264040 | Sequence: | 177264041 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Improvement of oxygen saturation | Measure | Improvement of quality of life | Measure | Improvement of exercise capacity | Measure | Improvement of phase angle |
Time Frame | 5 days | Time Frame | 5 days | Time Frame | 5 days | Time Frame | 5 days |
Description | Difference in oxygen saturation before first vs after last session | Description | Difference in CCQ score before first vs after last session | Description | Difference in 6-MWT outcome before first vs after last session | Description | Difference in oxygen saturation before first vs after last session |
Sponsors
Sequence: | 48290758 | Sequence: | 48290759 |
Agency Class | OTHER | Agency Class | UNKNOWN |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator |
Name | University Medical Center Groningen | Name | Tjongerschans hospital |
Central Contacts
Sequence: | 12000498 | Sequence: | 12000499 |
Contact Type | primary | Contact Type | backup |
Name | Jaap Westbroek | Name | Huib Kerstjens |
Phone | 0513-685227 | ||
j.westbroek@tjongerschans.nl | h.a.m.kerstjens@umcg.nl | ||
Role | Contact | Role | Contact |
Design Group Interventions
Sequence: | 68107533 | Sequence: | 68107534 |
Design Group Id | 55559415 | Design Group Id | 55559416 |
Intervention Id | 52454970 | Intervention Id | 52454971 |
Eligibilities
Sequence: | 30747756 |
Gender | All |
Minimum Age | 40 Years |
Maximum Age | 85 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
COPD patients, post-bronchodilator FEV1/FVC <70% and FEV1 <50% predicted Exclusion Criteria: Known malignant condition with limited life expectancy |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254122066 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 40 |
Maximum Age Num | 85 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 3 |
Designs
Sequence: | 30494039 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Triple |
Intervention Model Description | prospective, randomized, dubbel blind, placebo-controlled parallel study |
Subject Masked | True |
Caregiver Masked | True |
Investigator Masked | True |
Responsible Parties
Sequence: | 28860319 |
Responsible Party Type | Principal Investigator |
Name | Huib A.M. Kerstjens |
Title | Head of the department Pulmonary diseases and Tuberculosis |
Affiliation | University Medical Center Groningen |
]]>
https://zephyrnet.com/NCT03797781
2017-10-31
https://zephyrnet.com/?p=NCT03797781
NCT03797781https://www.clinicaltrials.gov/study/NCT03797781?tab=tableNANANAThe effect of different protein intakes on skeletal muscle atrophy during short term unilateral leg immobilisation.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2020-09-28 |
Start Month Year | October 31, 2017 |
Primary Completion Month Year | December 31, 2019 |
Verification Month Year | September 2020 |
Verification Date | 2020-09-30 |
Last Update Posted Date | 2020-09-28 |
Facilities
Sequence: | 200159416 |
Name | Sport and Health Science |
City | Exeter |
State | Devon |
Zip | EX1 2LU |
Country | United Kingdom |
Conditions
Sequence: | 52185496 |
Name | Muscle Atrophy |
Downcase Name | muscle atrophy |
Id Information
Sequence: | 40169077 |
Id Source | org_study_id |
Id Value | 6500619582 |
Countries
Sequence: | 42580668 |
Name | United Kingdom |
Removed | False |
Design Groups
Sequence: | 55609126 | Sequence: | 55609127 | Sequence: | 55609128 |
Group Type | Experimental | Group Type | Experimental | Group Type | Experimental |
Title | High protein | Title | Low protein | Title | Minimum protein |
Interventions
Sequence: | 52499438 |
Intervention Type | Other |
Name | Lower limb immobilisation (leg brace) with varying levels of protein intake |
Description | Single leg immobilisation via leg brace and crutches, the groups have different amounts of protein intake |
Design Outcomes
Sequence: | 177432050 | Sequence: | 177432051 |
Outcome Type | primary | Outcome Type | secondary |
Measure | Muscle size | Measure | Muscle strength |
Time Frame | 3 days | Time Frame | 3 days |
Browse Conditions
Sequence: | 193540163 | Sequence: | 193540164 | Sequence: | 193540165 | Sequence: | 193540166 | Sequence: | 193540167 | Sequence: | 193540168 |
Mesh Term | Muscular Atrophy | Mesh Term | Atrophy | Mesh Term | Pathological Conditions, Anatomical | Mesh Term | Neuromuscular Manifestations | Mesh Term | Neurologic Manifestations | Mesh Term | Nervous System Diseases |
Downcase Mesh Term | muscular atrophy | Downcase Mesh Term | atrophy | Downcase Mesh Term | pathological conditions, anatomical | Downcase Mesh Term | neuromuscular manifestations | Downcase Mesh Term | neurologic manifestations | Downcase Mesh Term | nervous system diseases |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48332341 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | University of Exeter |
Design Group Interventions
Sequence: | 68168188 | Sequence: | 68168189 | Sequence: | 68168190 |
Design Group Id | 55609126 | Design Group Id | 55609127 | Design Group Id | 55609128 |
Intervention Id | 52499438 | Intervention Id | 52499438 | Intervention Id | 52499438 |
Eligibilities
Sequence: | 30773581 |
Gender | Male |
Minimum Age | 18 Years |
Maximum Age | 35 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
BMI >18 and <28 no prescription medications or current illness. Exclusion Criteria: BMI <18 and >28 current prescription medication no history of leg injury. |
Adult | True |
Child | False |
Older Adult | False |
Calculated Values
Sequence: | 253952743 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Actual Duration | 26 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 35 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 1 |
Designs
Sequence: | 30519712 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Basic Science |
Time Perspective | |
Masking | Single |
Subject Masked | True |
Responsible Parties
Sequence: | 28886013 |
Responsible Party Type | Sponsor |
Study References
Sequence: | 52078924 |
Pmid | 32469388 |
Reference Type | derived |
Citation | Kilroe SP, Fulford J, Jackman S, Holwerda A, Gijsen A, van Loon L, Wall BT. Dietary protein intake does not modulate daily myofibrillar protein synthesis rates or loss of muscle mass and function during short-term immobilization in young men: a randomized controlled trial. Am J Clin Nutr. 2021 Mar 11;113(3):548-561. doi: 10.1093/ajcn/nqaa136. |
]]>
https://zephyrnet.com/NCT03797768
2019-12-25
https://zephyrnet.com/?p=NCT03797768
NCT03797768https://www.clinicaltrials.gov/study/NCT03797768?tab=tableNANANAChronic Obstructive Pulmonary Disease (COPD) is the fourth most important cause of death worldwide and is one of the commonest non-communicable diseases (NCDs) in Nepal. The presence of risk factors like indoor and outdoor air pollution, the high prevalence of smoking and lack of general awareness of COPD makes it a serious public health concern. However, no attempt has been made in Nepal to estimate its burden and address the disease at the community level. This community-based cluster randomized controlled study aims to fulfil that gap through mobilization of Female Community Health Workers (FCHVs) who will be trained to perform a certain set of health promotion activities aimed at prevention of the disease and its progression. Baseline and follow-up surveys will be conducted to compare the intervention and control groups. This study has the potential to generate evidence in helping address NCDs in Nepal and also other similar resource-limited countries.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2021-01-28 |
Start Month Year | December 25, 2019 |
Primary Completion Month Year | May 10, 2021 |
Verification Month Year | March 2020 |
Verification Date | 2020-03-31 |
Last Update Posted Date | 2021-01-28 |
Facilities
Sequence: | 200053304 |
Name | Aarhus University |
City | Aarhus |
Zip | 8000 |
Country | Denmark |
Conditions
Sequence: | 52156512 |
Name | Chronic Obstructive Pulmonary Disease |
Downcase Name | chronic obstructive pulmonary disease |
Id Information
Sequence: | 40148220 |
Id Source | org_study_id |
Id Value | AUTBA18 |
Countries
Sequence: | 42557739 |
Name | Denmark |
Removed | False |
Design Groups
Sequence: | 55577917 | Sequence: | 55577918 |
Group Type | Experimental | Group Type | No Intervention |
Title | Intervention | Title | Control |
Interventions
Sequence: | 52472019 |
Intervention Type | Behavioral |
Name | Behavioural-FCHV Visit |
Description | Female Community Health Volunteer will visit selected households on average 3 times a year for providing health promotion messages on improving lung health status and avoiding risk factors to COPD. |
Design Outcomes
Sequence: | 177328035 | Sequence: | 177328036 |
Outcome Type | primary | Outcome Type | secondary |
Measure | Forced Expiratory Volume in 1 second | Measure | Proportion of risk factors of COPD between intervention and control arm |
Time Frame | 1 year | Time Frame | 1 year |
Description | Mean difference in FVE1 between intervention and control arm |
Browse Conditions
Sequence: | 193432117 | Sequence: | 193432118 | Sequence: | 193432119 | Sequence: | 193432120 | Sequence: | 193432121 | Sequence: | 193432122 | Sequence: | 193432123 |
Mesh Term | Lung Diseases | Mesh Term | Lung Diseases, Obstructive | Mesh Term | Pulmonary Disease, Chronic Obstructive | Mesh Term | Respiratory Tract Diseases | Mesh Term | Chronic Disease | Mesh Term | Disease Attributes | Mesh Term | Pathologic Processes |
Downcase Mesh Term | lung diseases | Downcase Mesh Term | lung diseases, obstructive | Downcase Mesh Term | pulmonary disease, chronic obstructive | Downcase Mesh Term | respiratory tract diseases | Downcase Mesh Term | chronic disease | Downcase Mesh Term | disease attributes | Downcase Mesh Term | pathologic processes |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48306094 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | University of Aarhus |
Overall Officials
Sequence: | 29277937 |
Role | Principal Investigator |
Name | Tara Ballav Adhikari, MScPH |
Affiliation | Department of Public Health, Aarhus University, Aarhus, Denmark |
Design Group Interventions
Sequence: | 68130884 |
Design Group Id | 55577917 |
Intervention Id | 52472019 |
Eligibilities
Sequence: | 30757362 |
Gender | All |
Minimum Age | 40 Years |
Maximum Age | 90 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
Capable of performing spirometry Exclusion Criteria: Younger than 40 years of age |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254228065 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 40 |
Maximum Age Num | 90 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 1 |
Designs
Sequence: | 30503587 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Prevention |
Time Perspective | |
Masking | Single |
Outcomes Assessor Masked | True |
Links
Sequence: | 4386996 |
Url | https://doi.org/10.2147/COPD.S268110 |
Description | Prevalence of Chronic Obstructive Pulmonary Disease and its Associated Factors in Nepal: Findings from a Community-based Household Survey |
Responsible Parties
Sequence: | 28869865 |
Responsible Party Type | Sponsor |
Study References
Sequence: | 52049416 | Sequence: | 52049417 |
Pmid | 33061350 | Pmid | 34289879 |
Reference Type | background | Reference Type | derived |
Citation | Adhikari TB, Acharya P, Hogman M, Neupane D, Karki A, Drews A, Cooper BG, Sigsgaard T, Kallestrup P. Prevalence of Chronic Obstructive Pulmonary Disease and its Associated Factors in Nepal: Findings from a Community-based Household Survey. Int J Chron Obstruct Pulmon Dis. 2020 Sep 29;15:2319-2331. doi: 10.2147/COPD.S268110. eCollection 2020. | Citation | Adhikari TB, Neupane D, Karki A, Drews A, Cooper B, Hogman M, Sigsgaard T, Kallestrup P. Community-based intervention for prevention and management of chronic obstructive pulmonary disease in Nepal (COBIN-P trial): study protocol for a cluster-randomized controlled trial. Trials. 2021 Jul 21;22(1):474. doi: 10.1186/s13063-021-05447-7. |
]]>
https://zephyrnet.com/NCT03797755
2019-01-01
https://zephyrnet.com/?p=NCT03797755
NCT03797755https://www.clinicaltrials.gov/study/NCT03797755?tab=tableShing Fung Lee, MBBS (HK), FRCR (UK)leesfm@ha.org.hk852 2468 5087Many patients with incurable cancer will receive palliative oncological treatment before their death, and radiotherapy (RT) is an important element of this. The aim of palliative RT is to alleviate symptoms and improve quality of life. An accurate and practical survival prediction model for metastatic cancer patient receiving palliative RT can assist the decision making (ranging from best supportive treatment alone for expected short survival, to dose escalation for potential better disease control).
The available survival prediction models (such Survival Prediction Score using Number of Risk Factors by Chow et al and TEACHH model) have been developed in the Western world. We therefore perform a prospective observational study 1) to assess the overall survival of patients evaluated for palliative RT at a tertiary hospital in Hong Kong, and 2) to validate the prognostic score systems in our population.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-09 |
Start Month Year | January 1, 2019 |
Primary Completion Month Year | December 31, 2019 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-09 |
Facilities
Sequence: | 200244847 |
Status | Recruiting |
Name | Department of Clinical Oncology, Tuen Mun Hospital, Tuen Mun |
City | Hong Kong |
Country | Hong Kong |
Facility Contacts
Sequence: | 28128075 |
Facility Id | 200244847 |
Contact Type | primary |
Name | Shing Fung Lee, MBBS (HK), FRCR (UK) |
leesfm@ha.org.hk | |
Phone | 852 2468 5087 |
Conditions
Sequence: | 52208405 | Sequence: | 52208406 |
Name | Cancer | Name | Radiotherapy |
Downcase Name | cancer | Downcase Name | radiotherapy |
Id Information
Sequence: | 40186362 |
Id Source | org_study_id |
Id Value | NTWC_Onc_2019 |
Countries
Sequence: | 42599841 |
Name | Hong Kong |
Removed | False |
Design Groups
Sequence: | 55635012 |
Title | Palliative Cancer Patients |
Description | Stage IV cancer patients evaluated for palliative radiotherapy. |
Interventions
Sequence: | 52522369 |
Intervention Type | Radiation |
Name | palliative radiotherapy |
Description | Radiotherapy for palliating symptoms in stage IV cancer patients |
Keywords
Sequence: | 79923392 | Sequence: | 79923393 | Sequence: | 79923394 | Sequence: | 79923395 | Sequence: | 79923396 |
Name | survival | Name | cancer | Name | palliative | Name | radiotherapy | Name | prognosis |
Downcase Name | survival | Downcase Name | cancer | Downcase Name | palliative | Downcase Name | radiotherapy | Downcase Name | prognosis |
Design Outcomes
Sequence: | 177512384 | Sequence: | 177512385 | Sequence: | 177512386 | Sequence: | 177512387 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Overall Survival | Measure | Overall Survival in Each Indication of Palliative Radiotherapy | Measure | Overall Survival by Survival Prediction Model (NRF) | Measure | Overall Survival by Survival Prediction Model (TEACHH) |
Time Frame | 1 year | Time Frame | 3, 6, 9, 12 months | Time Frame | 3, 6, 9, 12 months | Time Frame | 3, 6, 9, 12 months |
Description | Overall Survival in the studied population | Description | Indications of Palliative Radiotherapy:
The indication will be as follow: spinal cord compression brain metastases tumor bleeding tumoral mass Cancer pain Superior Vena Cava Syndrome/ Airway compression |
Description | Overall Survival by Survival Prediction Score using Number of Risk Factors (NRF) | Description | Overall Survival by Survival Prediction Score using TEACHH Model |
Sponsors
Sequence: | 48354003 |
Agency Class | OTHER_GOV |
Lead Or Collaborator | lead |
Name | Tuen Mun Hospital |
Overall Officials
Sequence: | 29306143 |
Role | Principal Investigator |
Name | Shing Fung Lee, MBBS (HK), FRCR (UK) |
Affiliation | Department of Clinical Oncology, New Territory West Cluster, Hospital Authority, Hong Kong |
Central Contacts
Sequence: | 12017289 |
Contact Type | primary |
Name | Shing Fung Lee, MBBS (HK), FRCR (UK) |
Phone | 852 2468 5087 |
leesfm@ha.org.hk | |
Role | Contact |
Design Group Interventions
Sequence: | 68199602 |
Design Group Id | 55635012 |
Intervention Id | 52522369 |
Eligibilities
Sequence: | 30787045 |
Sampling Method | Non-Probability Sample |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Population | Stage IV cancer patients evaluated for palliative radiotherapy in Tuen Mun Hospital |
Criteria | Inclusion Criteria:
All adult patients with stage IV cancer who are referred for palliative RT in Tuen Mun Hospital, including both inpatients and outpatients. Exclusion Criteria: Patients who have received palliative RT before (i.e. not the first course palliative RT), have non-metastatic disease, are misclassified as palliative patients. |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253989941 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 3 |
Designs
Sequence: | 30533115 |
Observational Model | Cohort |
Time Perspective | Prospective |
Responsible Parties
Sequence: | 28899409 |
Responsible Party Type | Principal Investigator |
Name | Shing Fung Lee |
Title | Resident Specialist |
Affiliation | Tuen Mun Hospital |
Study References
Sequence: | 52103396 | Sequence: | 52103397 | Sequence: | 52103398 | Sequence: | 52103399 | Sequence: | 52103400 | Sequence: | 52103401 | Sequence: | 52103402 |
Pmid | 11527298 | Pmid | 10678857 | Pmid | 20564632 | Pmid | 19018082 | Pmid | 21263086 | Pmid | 29147245 | Pmid | 24122413 |
Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background |
Citation | Chow E, Harth T, Hruby G, Finkelstein J, Wu J, Danjoux C. How accurate are physicians' clinical predictions of survival and the available prognostic tools in estimating survival times in terminally ill cancer patients? A systematic review. Clin Oncol (R Coll Radiol). 2001;13(3):209-18. doi: 10.1053/clon.2001.9256. | Citation | Christakis NA, Lamont EB. Extent and determinants of error in doctors' prognoses in terminally ill patients: prospective cohort study. BMJ. 2000 Feb 19;320(7233):469-72. doi: 10.1136/bmj.320.7233.469. | Citation | Gripp S, Mjartan S, Boelke E, Willers R. Palliative radiotherapy tailored to life expectancy in end-stage cancer patients: reality or myth? Cancer. 2010 Jul 1;116(13):3251-6. doi: 10.1002/cncr.25112. | Citation | Chow E, Abdolell M, Panzarella T, Harris K, Bezjak A, Warde P, Tannock I. Predictive model for survival in patients with advanced cancer. J Clin Oncol. 2008 Dec 20;26(36):5863-9. doi: 10.1200/JCO.2008.17.1363. Epub 2008 Nov 17. | Citation | Peppercorn JM, Smith TJ, Helft PR, Debono DJ, Berry SR, Wollins DS, Hayes DM, Von Roenn JH, Schnipper LE; American Society of Clinical Oncology. American society of clinical oncology statement: toward individualized care for patients with advanced cancer. J Clin Oncol. 2011 Feb 20;29(6):755-60. doi: 10.1200/JCO.2010.33.1744. Epub 2011 Jan 24. | Citation | Chow E, James JL, Hartsell W, Scarantino CW, Ivker R, Roach M III, Suh JH, Demas W, Konski A, Bruner DW. Validation of a Predictive Model for Survival in Patients With Advanced Cancer: Secondary Analysis of RTOG 9714. World J Oncol. 2011 Aug;2(4):181-190. doi: 10.4021/wjon325w. Epub 2011 Aug 24. | Citation | Krishnan MS, Epstein-Peterson Z, Chen YH, Tseng YD, Wright AA, Temel JS, Catalano P, Balboni TA. Predicting life expectancy in patients with metastatic cancer receiving palliative radiotherapy: the TEACHH model. Cancer. 2014 Jan 1;120(1):134-41. doi: 10.1002/cncr.28408. Epub 2013 Oct 2. Erratum In: Cancer. 2019 Jul 1;125(13):2325. |
Ipd Information Types
Sequence: | 3336937 |
Name | Analytic Code |
]]>
https://zephyrnet.com/NCT03797742
2018-01-01
https://zephyrnet.com/?p=NCT03797742
NCT03797742https://www.clinicaltrials.gov/study/NCT03797742?tab=tableZhangwei Chenchen.zhangwei@zs-hospital.sh.cn+86 021 64041990Heart failure (HF), a current worldwide pandemic with an unacceptable high level of morbidity and mortality, brings an enormous medical and societal burden. Chronic HF is characterized by progressive alteration of cardiac structure and function. But the molecular mechanism of these alterations is still not well-established and needs to be discussed further. HF is a highly heterogeneous disease that can be caused by a multiple of diseases. Dilated cardiomyopathy (DCM) and ischemic cardiomyopathy (ICM) are the main causes of this syndrome. Although HF is the common manifestation of DCM and ICM, the etiology and pathogenesis are different. Understanding the different pathophysiological mechanisms will contribute to the prevention and individualized therapy of heart failure. Therefore, this study aims to observation the different characteristics of the molecular biology and clinical courses in DCM and ICM patients.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-01 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-09 |
Start Month Year | January 1, 2018 |
Primary Completion Month Year | December 1, 2022 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-09 |
Facilities
Sequence: | 200108787 |
Status | Recruiting |
Name | Zhongshan Hospital |
City | Shanghai |
Country | China |
Facility Contacts
Sequence: | 28106512 |
Facility Id | 200108787 |
Contact Type | primary |
Name | Zhangwei Chen |
chen.zhangwei@zs-hospital.sh.cn | |
Phone | +8602164041990 |
Conditions
Sequence: | 52171366 |
Name | Heart Failure |
Downcase Name | heart failure |
Id Information
Sequence: | 40158706 |
Id Source | org_study_id |
Id Value | HF201801 |
Countries
Sequence: | 42569031 |
Name | China |
Removed | False |
Design Groups
Sequence: | 55593293 | Sequence: | 55593294 | Sequence: | 55593295 |
Title | NC | Title | DCM | Title | ICM |
Description | Patients without heart failure. | Description | Dilated cardiomyopathy patients. | Description | Ischemic cardiomyopathy patients. |
Design Outcomes
Sequence: | 177379262 | Sequence: | 177379263 | Sequence: | 177379264 | Sequence: | 177379265 | Sequence: | 177379266 |
Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | NYHA functional class | Measure | All-cause mortality | Measure | hospitalization for cardiac causes | Measure | left ventricular end-diastolic dimension(LVEDD) dilates. | Measure | left ventricular ejection fraction reduces |
Time Frame | one year after enrolled | Time Frame | one year after enrolled | Time Frame | one year after enrolled | Time Frame | one year after enrolled | Time Frame | one year after enrolled |
Description | NYHA cardiac functional class | Description | All-cause mortality during follow-up | Description | hospitalization for cardiac causes during follow-up | Description | left ventricular structure changes:left ventricular end-diastolic dimension(LVEDD) dilates. | Description | left ventricular function changes:left ventricular ejection fraction reduces |
Browse Conditions
Sequence: | 193487183 | Sequence: | 193487184 | Sequence: | 193487185 |
Mesh Term | Heart Failure | Mesh Term | Heart Diseases | Mesh Term | Cardiovascular Diseases |
Downcase Mesh Term | heart failure | Downcase Mesh Term | heart diseases | Downcase Mesh Term | cardiovascular diseases |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48319401 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Shanghai Zhongshan Hospital |
Central Contacts
Sequence: | 12008908 |
Contact Type | primary |
Name | Zhangwei Chen |
Phone | +86 021 64041990 |
chen.zhangwei@zs-hospital.sh.cn | |
Role | Contact |
Eligibilities
Sequence: | 30765415 |
Sampling Method | Probability Sample |
Gender | All |
Minimum Age | 15 Years |
Maximum Age | 80 Years |
Healthy Volunteers | No |
Population | The inpatient in the department of cardiology of Zhongshan Hospital, Fudan University will be selected. |
Criteria | Inclusion Criteria:
LVEF≤ 55% Exclusion Criteria: Known malignant tumour diseases |
Adult | True |
Child | True |
Older Adult | True |
Calculated Values
Sequence: | 253889193 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 15 |
Maximum Age Num | 80 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 2 |
Number Of Secondary Outcomes To Measure | 3 |
Designs
Sequence: | 30511581 |
Observational Model | Case-Control |
Time Perspective | Prospective |
Responsible Parties
Sequence: | 28877876 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797729
2019-05-14
https://zephyrnet.com/?p=NCT03797729
NCT03797729https://www.clinicaltrials.gov/study/NCT03797729?tab=tableHongyi Wu, MDwu.hongyi@zs-hospital.sh.cn+8602164041990Anti-platelet therapy is a key point of acute myocardial infarction (AMI) treatment. Nowadays, dual anti-platelet therapy based on aspirin and ADP-P2Y12 receptor inhibitor is the preferred treatment before primary percutaneous coronary intervention (PPCI). Restricted by pharmacokinetic and pharmacodynamic characteristics, ADP-P2Y12 receptor inhibitors cannot take effect immediately after oral administration. However, platelet glycoprotein Ⅱb / Ⅲa inhibitors take effect faster. Previous clinical trials indicated that combination of full dose of glycoprotein Ⅱb / Ⅲa inhibitor and dual anti-platelet therapy reduced AMI related ischemia events but increased bleeding events significantly. The high dose of glycoprotein Ⅱb / Ⅲa inhibitor may be the key factor contributing to the increased bleeding events. Therefore, this study aims to evaluate the effectiveness and security of triple anti-platelet therapy based on a small dose of glycoprotein Ⅱb / Ⅲa inhibitor, aspirin and ADP-P2Y12 receptor inhibitor in AMI patients receiving PPCI.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-01 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2020-01-22 |
Start Month Year | May 14, 2019 |
Primary Completion Month Year | June 2021 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2020-01-22 |
Facilities
Sequence: | 200280881 |
Status | Recruiting |
Name | Zhongshan Hospital Fudan University |
City | Shanghai |
State | Shanghai |
Zip | 200032 |
Country | China |
Facility Contacts
Sequence: | 28132928 | Sequence: | 28132929 |
Facility Id | 200280881 | Facility Id | 200280881 |
Contact Type | primary | Contact Type | backup |
Name | Zhangwei Chen, MD | Name | Danbo Lu, PhD |
chen.zhangwei@zs-hospital.sh.cn | lu.danbo@zs-hospital.sh.cn | ||
Phone | +86 21 64041990 | Phone | +86 21 64041990 |
Browse Interventions
Sequence: | 96133493 | Sequence: | 96133494 | Sequence: | 96133495 | Sequence: | 96133496 | Sequence: | 96133497 |
Mesh Term | Tirofiban | Mesh Term | Fibrinolytic Agents | Mesh Term | Fibrin Modulating Agents | Mesh Term | Molecular Mechanisms of Pharmacological Action | Mesh Term | Platelet Aggregation Inhibitors |
Downcase Mesh Term | tirofiban | Downcase Mesh Term | fibrinolytic agents | Downcase Mesh Term | fibrin modulating agents | Downcase Mesh Term | molecular mechanisms of pharmacological action | Downcase Mesh Term | platelet aggregation inhibitors |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Conditions
Sequence: | 52221783 |
Name | ST Elevation Myocardial Infarction |
Downcase Name | st elevation myocardial infarction |
Id Information
Sequence: | 40195804 |
Id Source | org_study_id |
Id Value | TRYIT |
Countries
Sequence: | 42609784 |
Name | China |
Removed | False |
Design Groups
Sequence: | 55650069 | Sequence: | 55650070 |
Group Type | Placebo Comparator | Group Type | Experimental |
Title | Normal saline | Title | Tirofiban |
Interventions
Sequence: | 52535578 | Sequence: | 52535579 |
Intervention Type | Drug | Intervention Type | Drug |
Name | Tirofiban | Name | Normal saline |
Description | Upon being diagnosed as ST Elevation Myocardial Infarction, if informed consent is obtained, patients start to receive Tirofiban(0.05mg/ml) intravenous drip in a dosage of 4ml/hour (patients weight<50kg) or 6ml/hour (patients weight > 50kg) lasting for 24 hours. | Description | Upon being diagnosed as ST Elevation Myocardial Infarction, if informed consent is obtained, patients start to receive normal saline intravenous drip in a dosage of 4ml/hour (patients weight<50kg) or 6ml/hour (patients weight > 50kg) lasting for 24 hours. |
Keywords
Sequence: | 79942103 | Sequence: | 79942104 | Sequence: | 79942105 |
Name | ST Elevation Myocardial Infarction | Name | Tirofiban | Name | Percutaneous Coronary Intervention |
Downcase Name | st elevation myocardial infarction | Downcase Name | tirofiban | Downcase Name | percutaneous coronary intervention |
Design Outcomes
Sequence: | 177562272 | Sequence: | 177562273 | Sequence: | 177562274 | Sequence: | 177562275 | Sequence: | 177562276 | Sequence: | 177562277 | Sequence: | 177562278 | Sequence: | 177562279 | Sequence: | 177562280 | Sequence: | 177562281 | Sequence: | 177562282 | Sequence: | 177562283 | Sequence: | 177562284 |
Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other |
Measure | TFG(TIMI flow grades) grade III: complete myocardial perfusion immediately after primary percutaneous coronary intervention detected by DSA(Digital Substraction Angiography). | Measure | TMP(TIMI myocardial perfusion grades) grade III: complete myocardial perfusion immediately after primary percutaneous coronary intervention detected by DSA(Digital Substraction Angiography). | Measure | Remedial Tirofiban intravenous use during primary percutaneous coronary intervention procedure. | Measure | ST segment | Measure | Myocardial microcirculation perfusion estimated by cardiac magnetic (CMR). | Measure | Major adverse cardiovascular events(MACE), including a composite of all-cause death, nonfatal myocardial infarction, stroke, target vessel revascularization. | Measure | Left ventricular ejection fraction (LVEF) assessed by transthoracic echocardiography. | Measure | The serum microRNA expression pattern changes after primary percutaneous coronary intervention. | Measure | All the bleeding events assessed by bleeding academic research consortium(BARC) definition for bleeding) | Measure | Major bleeding events assessed by TIMI bleeding criteria. | Measure | Severe or life-threatening and moderate bleeding events assessed by GUSTO bleeding criteria. | Measure | Major bleeding events assessed by international society on thrombosis and haemostasis(ISTH) bleeding criteria. | Measure | Adverse events and severe adverse events. |
Time Frame | Immediately after primary percutaneous coronary intervention. | Time Frame | Immediately after primary percutaneous coronary intervention. | Time Frame | During the process of primary percutaneous coronary intervention. | Time Frame | 90 minutes after primary percutaneous coronary intervention. | Time Frame | 7 days after primary percutaneous coronary intervention. | Time Frame | 30 days after primary percutaneous coronary intervention. | Time Frame | 7 and 30 days after primary percutaneous coronary intervention. | Time Frame | Pre-, 30 minutes, 3 hours and 24 hours after primary percutaneous coronary intervention. | Time Frame | 30 days after primary percutaneous coronary intervention. | Time Frame | 30 days after primary percutaneous coronary intervention. | Time Frame | 30 days after primary percutaneous coronary intervention. | Time Frame | 30 days after primary percutaneous coronary intervention. | Time Frame | 30 days after primary percutaneous coronary intervention. |
Description | TIMI flow grades: grade III. | Description | TIMI myocardial perfusion grades: grade III. | Description | Remedial Tirofiban use during primary percutaneous coronary intervention. | Description | The sum of the initial ST segment elevation drops 70% or more. | Description | Myocardial microcirculation perfusion estimated by cardiac magnetic resonance imaging. | Description | Major adverse cardiovascular events, including a composite of all-cause death, nonfatal myocardial infarction, stroke, target vessel revascularization. | Description | Left ventricular ejection fraction assessed by transthoracic echocardiography. | Description | The microRNA expression pattern changes. | Description | All the bleeding events assessed by bleeding academic research consortium(BARC) definition for bleeding) | Description | Any intracranial bleeding (excluding microhemorrhages <10 mm evident only on gradient-echo MRI); Clinically overt signs of hemorrhage associated with a drop in hemoglobin of ≥ 5 g/dL; Fatal bleeding (bleeding that directly results in death within 7 d). | Description | GUSTO bleeding criteria:Severe or life-threatening :
Intracerebral hemorrhage ; Resulting in substantial hemodynamic compromise requiring treatment. Moderate: Requiring blood transfusion but not resulting in hemodynamic compromise. Mild : Bleeding that does not meet above criteria. |
Description | Fatal bleeding and/or symptomatic bleeding in a critical area or organ such as intracranial, intraspinal, intraocular, retroperitoneal, intra-articular or pericardial, or intramuscular with compartment syndrome, and/or bleeding causing hemoglobin drop of 20 g/L or more, and/or blood transfusion of 2 units or more | Description | Adverse events and severe adverse events. |
Browse Conditions
Sequence: | 193679412 | Sequence: | 193679413 | Sequence: | 193679414 | Sequence: | 193679415 | Sequence: | 193679416 | Sequence: | 193679417 | Sequence: | 193679418 | Sequence: | 193679419 | Sequence: | 193679420 | Sequence: | 193679421 |
Mesh Term | Myocardial Infarction | Mesh Term | ST Elevation Myocardial Infarction | Mesh Term | Infarction | Mesh Term | Ischemia | Mesh Term | Pathologic Processes | Mesh Term | Necrosis | Mesh Term | Myocardial Ischemia | Mesh Term | Heart Diseases | Mesh Term | Cardiovascular Diseases | Mesh Term | Vascular Diseases |
Downcase Mesh Term | myocardial infarction | Downcase Mesh Term | st elevation myocardial infarction | Downcase Mesh Term | infarction | Downcase Mesh Term | ischemia | Downcase Mesh Term | pathologic processes | Downcase Mesh Term | necrosis | Downcase Mesh Term | myocardial ischemia | Downcase Mesh Term | heart diseases | Downcase Mesh Term | cardiovascular diseases | Downcase Mesh Term | vascular diseases |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48366645 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Shanghai Zhongshan Hospital |
Overall Officials
Sequence: | 29313022 |
Role | Study Chair |
Name | Juying Qian, MD |
Affiliation | Fudan University |
Central Contacts
Sequence: | 12020642 | Sequence: | 12020643 |
Contact Type | primary | Contact Type | backup |
Name | Zhangwei Chen, MD | Name | Hongyi Wu, MD |
Phone | +8602164041990 | Phone | +8602164041990 |
chen.zhangwei@zs-hospital.sh.cn | wu.hongyi@zs-hospital.sh.cn | ||
Phone Extension | 612747 | ||
Role | Contact | Role | Contact |
Design Group Interventions
Sequence: | 68217714 | Sequence: | 68217715 |
Design Group Id | 55650070 | Design Group Id | 55650069 |
Intervention Id | 52535578 | Intervention Id | 52535579 |
Eligibilities
Sequence: | 30794853 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 85 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Time after onset of chest pain: ≥ 30 minutes and ≤ 24 hours; Exclusion Criteria: Life expectancy ≤ 1 year; |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254004536 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 85 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 2 |
Number Of Secondary Outcomes To Measure | 4 |
Number Of Other Outcomes To Measure | 7 |
Designs
Sequence: | 30540893 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Double |
Subject Masked | True |
Outcomes Assessor Masked | True |
Intervention Other Names
Sequence: | 26697027 |
Intervention Id | 52535579 |
Name | Sodium Chloride Injection |
Responsible Parties
Sequence: | 28907213 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797716
2019-03-01
https://zephyrnet.com/?p=NCT03797716
NCT03797716https://www.clinicaltrials.gov/study/NCT03797716?tab=tableChristopher R Evans, MBBSsitu.littlejourney@ucl.ac.uk02076799280To evaluate the clinical effectiveness of a virtual reality psychological preparation app at reducing peri-operative anxiety and its associated sequelae in children aged 3-12 years old undergoing ambulatory surgery compared to standard care.
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Studies
Study First Submitted Date | 2018-11-23 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-09 |
Start Month Year | March 1, 2019 |
Primary Completion Month Year | September 30, 2020 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-09 |
Detailed Descriptions
Sequence: | 20710007 |
Description | This is a phase III multi-centre randomised controlled trial evaluating the effectiveness of the Little Journey app: a pre-hospital psychological preparation tool designed for children undergoing ambulatory surgery.
Children presenting to the Preoperative assessment clinic before their operation will be screened for recruitment to the trial. Those meeting the inclusion criteria will be recruited to participate in the trial before randomisation into either a standard practice arm or intervention arm. Consent will be provided by parents / guardians and assent by children aged 7-12 years old. Children assigned to the intervention arm will be provided with a virtual reality google cardboard headset and access code for the Little Journey app which they can use as many times as they wish before their operation. They will also receive the standard pre-operative preparation and care as per the recruiting site. In comparison, the standard care arm will receive a google cardboard virtual reality headset with suggestions of free virtual apps to use and standard pre-operative preparation and care – as defined by each participating site. Children's anxiety will be assessed at multiple time points along the surgical journey, ranging from the preoperative assessment clinic, ward and finally in the anaesthetic room during the induction of anaesthesia. Secondary outcome measures such as parent anxiety levels, post-hospital behavioural changes, need for rescue analgesia and antiemetics in the recovery room will be recorded. Children's anxiety scores in those assigned to the intervention arm will undergo a further analysis assessing the impact of frequency and timing of Little Journey app use before surgery. |
Conditions
Sequence: | 52139051 | Sequence: | 52139052 | Sequence: | 52139053 | Sequence: | 52139054 | Sequence: | 52139055 | Sequence: | 52139056 |
Name | Anxiety Acute | Name | Anxiety Fear | Name | Peri-operative | Name | Psychological Distress | Name | Surgery | Name | Children, Only |
Downcase Name | anxiety acute | Downcase Name | anxiety fear | Downcase Name | peri-operative | Downcase Name | psychological distress | Downcase Name | surgery | Downcase Name | children, only |
Id Information
Sequence: | 40135101 |
Id Source | org_study_id |
Id Value | 18/0197 |
Design Groups
Sequence: | 55559408 | Sequence: | 55559409 |
Group Type | No Intervention | Group Type | Experimental |
Title | Standard Care arm | Title | Intervention arm |
Description | Participants will receive standard of care from the pre-assessment clinic until discharge.
A typical preparatory National Health Service pathway would include: meeting a specialist nurse in the preoperative assessment clinic; a preoperative anaesthetic and surgical consultation; interaction with health play specialists on the day of surgery; and distraction interventions such as hand-held tablets during induction of anaesthesia. Participants may have inhalation or intravenous induction depending on the primary management plan of the anaesthetist in charge. Participants in the standard care arm will also receive a virtual reality cardboard headset, which can be taken home, personalised and decorated before use with virtual reality apps available to download from the app stores. |
Description | Participants allocated to the intervention arm will receive the same peri-operative management as the standard care arm and will also receive an access code enabling them to use the Little Journey app in the weeks leading up to their operation. We suggest the Little Journey app is used in the days to weeks leading up to the child's operation depending on their age. On downloading the app, if parents/carers insert the age of the child and date of surgery into the Little Journey app they will be sent a push notifications reminding them when to use it according to their child's age. However, it can be used as frequently as the child and/or their parents or carers wish before the operation. |
Interventions
Sequence: | 52454964 |
Intervention Type | Device |
Name | Little Journey app |
Description | The Little Journey app allows children to explore 360-degree hospital environments familiarising and desensitising them to areas and staff they'll see on the day of surgery. Children can "visit" the day case ward, anaesthetic and recovery rooms where their operation will occur -all while feeling safe in their own home. As the child explores the three areas, they are introduced to animated characters of staff who explain what will happen, the equipment that will be used and how they might feel. Using head tracking technology, the child triggers the animated characters by looking at them; meaning they control the pace of learning and speed at which they progress. The preparatory tool follows a pre-set story-line reflecting what happens from admission to discharge on the day of surgery. |
Keywords
Sequence: | 79822888 |
Name | Anxiety, peri-operative, preparation, app |
Downcase Name | anxiety, peri-operative, preparation, app |
Design Outcomes
Sequence: | 177264013 | Sequence: | 177264027 | Sequence: | 177264014 | Sequence: | 177264015 | Sequence: | 177264016 | Sequence: | 177264017 | Sequence: | 177264018 | Sequence: | 177264019 | Sequence: | 177264020 | Sequence: | 177264021 | Sequence: | 177264022 | Sequence: | 177264023 | Sequence: | 177264024 | Sequence: | 177264025 | Sequence: | 177264026 | Sequence: | 177264028 | Sequence: | 177264029 | Sequence: | 177264030 | Sequence: | 177264031 | Sequence: | 177264032 | Sequence: | 177264033 | Sequence: | 177264034 | Sequence: | 177264035 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Modified Yale Pre Operative Anxiety score (shortened form) | Measure | Virtual reality headset side effects | Measure | Modified Yale Pre Operative Anxiety score (shortened form) | Measure | Parent anxiety levels | Measure | Modified Yale Pre Operative Anxiety score (shortened form) | Measure | Parent satisfaction with pre-operative information | Measure | Child compliance in the anaesthetic room | Measure | Child distress in the anaesthetic room | Measure | Parent anxiety levels | Measure | Time to induction of anaesthesia | Measure | Incidence of the need for premedication | Measure | Analgesia and anti-emetic use in the recovery room. | Measure | Time to recovery readiness | Measure | Parent satisfaction with care | Measure | Time spent in hospital | Measure | Incidence of unplanned admissions to hospital following surgery | Measure | Incidence of unplanned cancellations on the scheduled date of surgery. | Measure | Post Hospital Behavioural Questionnaire | Measure | Social cost analysis (Parents/Guardian) | Measure | Social cost analysis (Participants) | Measure | Post Hospital Behavioural Questionnaire | Measure | Social cost analysis (Parents/Guardian) | Measure | Social cost analysis (Participants) |
Time Frame | Day of surgery (Day 1): Measured during the induction of anaesthesia in the anaesthetic room | Time Frame | Day of Surgery (Day 1): Non-validated questionnaire completed immediately prior to discharge from hospital | Time Frame | Two weeks to six months before surgery: mYPAS-SF measured pre-randomisation in the Pre-Assessment clinic occurring a minimum of two-weeks before surgery, up to six-months before surgery depending on the participating research site. | Time Frame | Two-weeks to six-months before surgery: Measured pre-randomisation in the pre-assessment clinic occurring a minimum of two-weeks before surgery, up to six-months before surgery date depending on the participating research site. | Time Frame | Day of Surgery (Day 1): Measured on the ward prior to surgery | Time Frame | Day of Surgery (Day 1): Measured on the ward prior to the operation on the day of surgery. | Time Frame | Day of surgery (Day 1): Recorded immediately following observation of the induction of anaesthesia | Time Frame | Day of surgery (Day 1): Recorded immediately following observation of the induction of anaesthesia | Time Frame | Day of surgery (Day 1): Measured immediately following observation of the induction of anaesthesia. | Time Frame | Day of surgery (Day 1): Measured from entry into the anaesthetic room to entry into theatre. | Time Frame | Day of surgery (Day 1): As recorded in the anaesthetic room | Time Frame | Day of surgery (Day 1): Recorded in the recovery room following surgery | Time Frame | Day of surgery (Day 1): Measured from patients arrival in the recovery room until deemed ready for discharge. | Time Frame | Day of surgery (Day 1): Measured on the ward prior to discharge home following surgery. | Time Frame | Day of surgery (Day 1): Recorded at end of day of surgery following discharge. | Time Frame | Day of surgery (Day 1): Recorded at end of day of surgery | Time Frame | Day of surgery (Day 1): Recorded on the day of surgery | Time Frame | Day 14 post surgery: Completed at two-weeks after surgery by telephone consultation with parents/guardians | Time Frame | Day 14 post surgery: Completed at two-weeks after surgery by telephone consultation with parents/guardians | Time Frame | Day 14 post surgery: Completed at two-weeks after surgery by telephone consultation with parents/guardians | Time Frame | Day 28 post surgery: Completed at four-weeks after surgery by telephone consultation with parents/guardians | Time Frame | Day 28 post surgery: Completed at four-weeks after surgery by telephone consultation with parents/guardians | Time Frame | Day 28 post surgery: Completed at four-weeks after surgery by telephone consultation with parents/guardians |
Description | An independent and blinded observer completed observational scoring tool. Children are scored in four categories: Activity, vocalisations, emotional expressivity and state of apparent arousal, according to pre-determined Likert scale observations. Each category score is divided by its highest possible score, before being added together; these scores are then divided by four and multiplied by 100, giving a value between 22.92 to 100. Higher values indicate greater anxiety levels, with scores greater than 30 typically representing clinically significant anxiety. | Description | An assessment of the side effects of use of a virtual reality headset in both children and their parents assessed through a parent reported checkbox questionnaire. | Description | An independent and blinded observer completed observational scoring tool. Children are scored in four categories: Activity, vocalisations, emotional expressivity and state of apparent arousal, according to pre-determined Likert scale observations. Each category score is divided by its highest possible score, before being added together; these scores are then divided by four and multiplied by 100, giving a value between 22.92 to 100. Higher values indicate greater anxiety levels, with scores greater than 30 typically representing clinically significant anxiety. | Description | A 100mm visual analogue scale assessing the current anxiety levels of parents (VAS-PA) about their child's surgery. The VAS-PA is a rapid method of assessing self-reported anxiety levels of parents before surgery. Self reported scores range from 0-100mm with higher scores signifying greater anxiety. | Description | An independent and blinded observer completed observational scoring tool. Children are scored in four categories: Activity, vocalisations, emotional expressivity and state of apparent arousal, according to pre-determined Likert scale observations. Each category score is divided by its highest possible score, before being added together; these scores are then divided by four and multiplied by 100, giving a value between 22.92 to 100. Higher values indicate greater anxiety levels, with scores greater than 30 typically representing clinically significant anxiety. | Description | A 100mm visual analogue scale assessing parents' satisfaction with the pre-operative information. This parent-reported score ranges from 0-100mm with higher scores signifying higher levels of satisfaction. | Description | A 100mm visual analogue scale assessing the child's compliance during the induction of anaesthesia completed by the independent observer following observation of the induction of anaesthesia. This independent observer reported score ranges from 0-100mm with higher scores signifying higher levels of compliance. | Description | A 100mm visual analogue scale assessing the child's level of distress during the induction of anaesthesia completed by the independent observer following observation of the induction of anaesthesia. This independent observer reported score ranges from 0-100mm with higher scores signifying higher levels of distress during the induction. | Description | A 100mm visual analogue scale assessing the current anxiety levels of parents (VAS-PA) about their child's surgery. The VAS-PA is a rapid method of assessing self-reported anxiety levels of parents before surgery. Self reported scores range from 0-100mm with higher scores signifying greater anxiety. | Description | The time taken for the induction of anaesthesia (minutes) | Description | Number of patients given premedication prior to the induction of anaesthesia as per the prescription of the anaesthetist. | Description | As directed by the trial arm blinded clinical team based on their perceptions of child's symptoms in the recovery room. | Description | The time taken for participant to be ready for discharge back to the ward from the recovery room (minutes) as deemed by the recovery room nursing staff. | Description | A 100mm visual analogue scale assessing parents' satisfaction with the care they received on the day of surgery. This parent-reported score ranges from 0-100mm with higher scores signifying higher levels of satisfaction. | Description | The total time the participant spend in hospital from arrival on the ward to being discharged home (minutes). | Description | The number of participants requiring unplanned admission to hospital following surgery for any reason. | Description | The number of participants whose surgery is cancelled on the day of surgery for any reason. | Description | A parent-completed eleven-point questionnaire assessing changes in their child's behaviour following surgery. Consisting of eleven items, each item is scored using a five-point Likert scale ranging from "much less than before" to " much more than before". Higher scores are suggestive of increased post hospital regressive behavioural changes. | Description | The number of combined days of work missed by Parents/guardians following their child's surgery. Higher numbers are indicative of increased social costs. | Description | The number of days of school missed by children following their surgery. Higher numbers are indicative of increased social costs. | Description | A parent-completed eleven-point questionnaire assessing changes in their child's behaviour following surgery. Consisting of eleven items, each item is scored using a five-point Likert scale ranging from "much less than before" to " much more than before". Higher scores are suggestive of increased post hospital regressive behavioural changes. | Description | The number of combined days of work missed by Parents/guardians following their child's surgery. Higher numbers are indicative of increased social costs. | Description | The number of days of school missed by children following their surgery. Higher numbers are indicative of increased social costs. |
Browse Conditions
Sequence: | 193366740 | Sequence: | 193366741 |
Mesh Term | Anxiety Disorders | Mesh Term | Mental Disorders |
Downcase Mesh Term | anxiety disorders | Downcase Mesh Term | mental disorders |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48290753 | Sequence: | 48290754 |
Agency Class | OTHER | Agency Class | OTHER_GOV |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator |
Name | University College, London | Name | National Institute for Health Research, United Kingdom |
Overall Officials
Sequence: | 29268555 |
Role | Study Chair |
Name | Ramani S Moonesinghe, MBBS, MRCP, FRCA, FFICM, MD |
Affiliation | University College, London |
Central Contacts
Sequence: | 12000497 |
Contact Type | primary |
Name | Christopher R Evans, MBBS |
Phone | 02076799280 |
situ.littlejourney@ucl.ac.uk | |
Role | Contact |
Design Group Interventions
Sequence: | 68107526 |
Design Group Id | 55559409 |
Intervention Id | 52454964 |
Eligibilities
Sequence: | 30747753 |
Gender | All |
Minimum Age | 3 Years |
Maximum Age | 12 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
Children aged between 3-12 years of age on the date of parental consent to participate in the trial Note: Surgery is defined as any procedure occurring in a theatre under the care of a surgeon or dentist and an anaesthetist. Exclusion Criteria: Children aged less than 3 years of age or more than 12 years' old on the date of parental consent Note: Children undergoing diagnostic procedures (e.g. MRI, Cardiac catheterisation) will not be included due to diagnostic uncertainty. |
Adult | False |
Child | True |
Older Adult | False |
Calculated Values
Sequence: | 254122019 |
Registered In Calendar Year | 2018 |
Were Results Reported | False |
Has Single Facility | False |
Minimum Age Num | 3 |
Maximum Age Num | 12 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 22 |
Designs
Sequence: | 30494036 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Health Services Research |
Time Perspective | |
Masking | Double |
Caregiver Masked | True |
Outcomes Assessor Masked | True |
Responsible Parties
Sequence: | 28860316 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797703
2018-11-26
https://zephyrnet.com/?p=NCT03797703
NCT03797703https://www.clinicaltrials.gov/study/NCT03797703?tab=tableNANANAThis is a prospective study to assess the utility of Lidocaine Hydrochloride 2% gel enema (Hi-Tech Pharmacal Co., Inc.) in reducing post-procedural pain after endoscopic band ligation of internal hemorrhoids. Briefly, patients will be consented prior to entry into the study. During the endoscopic band ligation procedure, patients will be blindly placed into the treatment arm or control arm. The treatment arm will receive 15 ml enema of lidocaine gel immediately upon cessation of the procedure. In the placebo arm, oral pain medications will be provided. Researchers will assess pain following the procedure at 1 hour, 24 hours and 48 hours via telephone call. Another telephone call will be performed at 72 to 96 hours to assess any side effects of the medication.
<![CDATA[
Studies
Study First Submitted Date | 2018-12-19 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2020-11-25 |
Start Month Year | November 26, 2018 |
Primary Completion Month Year | May 29, 2020 |
Verification Month Year | November 2020 |
Verification Date | 2020-11-30 |
Last Update Posted Date | 2020-11-25 |
Detailed Descriptions
Sequence: | 20727181 |
Description | This is a prospective single center study to evaluate side effects and efficacy of a lidocaine jelly 2% enema following endoscopic hemorrhoid band ligation. The investigators will administer a single dose of 15 mL lidocaine jelly 2%, obtained from Advocate main pharmacy, as an enema immediately post procedure. Patients will not be permitted to self-administer additional doses following discharge.
Prior to being enrolled in the study, the clinician will perform a Comprehensive Metabolic Panel and Complete Blood Count. When appropriate, a urine pregnancy test will be performed prior to enrollment. The investigators will assess for any signs or symptoms of liver disease. These assessments will occur within one month of the procedure date. If the patient has any signs of renal or hepatic impairment (creatinine greater than 2 or Childs Pugh Class 3), they will be excluded from the study. The researchers will also exclude patients with any history of arrhythmias or who are currently on anti-arrhythmic medications. Once the patient is deemed safe to proceed, the lidocaine gel enema will be placed at the cessation of the procedure by the investigator. At the time of the procedure, the clinician will assess and use their best judgement to determine if the rectal mucosa is generally intact by visual inspection. If the mucosa remains intact, the subject will be able to be included in the study. However, if the rectal mucosa is traumatized the subject will be excluded and will not participate in the randomized treatment. Following the procedure, the patient will be monitored closely with a one-on one registered nurse for 4 hours in an observation unit. Vital signs will be taken every 5 minutes, as well as continuous EKG monitoring and pulse oximetry monitoring. If any adverse side effects occur, the physician is immediately available for further management and admission to the hospital if needed. Upon completion of the 4-hour observation period, the participants will be evaluated by a registered nurse and physician prior to discharge home following the procedure. The patient will be discharged with a responsible adult who will care for the patient for 24 additional hours. The clinician will communicate with the patient and responsible adult regarding any adverse side effects. The patient will also receive a phone number to call to reach the physician or the physician's associate who will be able to verbally assist the patient immediately should any adverse events occur. For data collection, one hour following the procedure a clinician will screen for any adverse side effects and pain will be assessed using a numeric pain scale (0-10). The patient will also be contacted via telephone to assess adverse side effects and pain scale at 24 hours and 48 hours post procedure. The investigators will also call the patient at 72 to 96 hours to assess for any adverse effects. The patients will be followed up by the principal investigator for routine check-ups following the procedure. The clinician will be easily accessible via telephone and the patient will be given instructions on how to contact the clinician, if needed. Data to be collected on each subject will include: date of procedure, specific patient ID, gender, age, internal hemorrhoids grade, race (White, African American, Hispanic, Asian), BMI, comorbid conditions, pain 1 hour post procedure, pain 24 and 48 hours post procedure, requirement of narcotic pain medication, requirement of other oral analgesic medication, sedation utilized and complications or adverse side effects from the medication. Upon data collection of this trial, we will monitor for any adverse events. If there is an adverse event that is deemed by the principal investigator likely due to drug administration, we will report it to the FDA immediately through written communication and an IND Safety Report. It will be reported within at least 7 calendar days of being notified of the adverse event. |
Facilities
Sequence: | 200159414 |
Name | Advocate Christ Medical Center |
City | Oak Lawn |
State | Illinois |
Zip | 60453 |
Country | United States |
Browse Interventions
Sequence: | 96074169 | Sequence: | 96074170 | Sequence: | 96074171 | Sequence: | 96074172 | Sequence: | 96074173 | Sequence: | 96074174 | Sequence: | 96074175 | Sequence: | 96074176 | Sequence: | 96074177 | Sequence: | 96074178 | Sequence: | 96074179 | Sequence: | 96074180 |
Mesh Term | Lidocaine | Mesh Term | Anesthetics, Local | Mesh Term | Anesthetics | Mesh Term | Central Nervous System Depressants | Mesh Term | Physiological Effects of Drugs | Mesh Term | Sensory System Agents | Mesh Term | Peripheral Nervous System Agents | Mesh Term | Anti-Arrhythmia Agents | Mesh Term | Voltage-Gated Sodium Channel Blockers | Mesh Term | Sodium Channel Blockers | Mesh Term | Membrane Transport Modulators | Mesh Term | Molecular Mechanisms of Pharmacological Action |
Downcase Mesh Term | lidocaine | Downcase Mesh Term | anesthetics, local | Downcase Mesh Term | anesthetics | Downcase Mesh Term | central nervous system depressants | Downcase Mesh Term | physiological effects of drugs | Downcase Mesh Term | sensory system agents | Downcase Mesh Term | peripheral nervous system agents | Downcase Mesh Term | anti-arrhythmia agents | Downcase Mesh Term | voltage-gated sodium channel blockers | Downcase Mesh Term | sodium channel blockers | Downcase Mesh Term | membrane transport modulators | Downcase Mesh Term | molecular mechanisms of pharmacological action |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Conditions
Sequence: | 52185494 |
Name | Hemorrhoids |
Downcase Name | hemorrhoids |
Id Information
Sequence: | 40169075 |
Id Source | org_study_id |
Id Value | AHC-6999-M5000223 |
Countries
Sequence: | 42580666 |
Name | United States |
Removed | False |
Design Groups
Sequence: | 55609122 | Sequence: | 55609123 |
Group Type | Experimental | Group Type | No Intervention |
Title | Treatment | Title | Control |
Description | Patients will be randomly allocated into the treatment group. The treatment group will receive a 15 mL lidocaine gel enema rectally immediately following completion of the procedure. | Description | Patients will be randomly allocated into the control group. The control group will not receive a rectal enema. |
Interventions
Sequence: | 52499435 |
Intervention Type | Drug |
Name | Lidocaine Hydrochloride 2% gel enema |
Description | Insertion of Lidocaine Hydrochloride 2% gel enema rectally immediately following the procedure. |
Design Outcomes
Sequence: | 177432042 | Sequence: | 177432043 |
Outcome Type | primary | Outcome Type | secondary |
Measure | Change in Pain following Procedure at 1 hour, 24 hours and 48 hours | Measure | Pain Medication Needs |
Time Frame | This information will be collected at 1 hour, 24 hours and 48 hours after the procedure. | Time Frame | This will be evaluated 48 hours after the procedure. |
Description | This effect will be measured by statistical analysis comparing the treatment groups numeric pain scale ratings (0-10) with the control groups numeric pain scale ratings (0-10). | Description | This effect will be measured by asking the subject what pain medication was needed following the procedure and the amount taken. |
Browse Conditions
Sequence: | 193540144 | Sequence: | 193540145 | Sequence: | 193540146 | Sequence: | 193540147 | Sequence: | 193540148 | Sequence: | 193540149 | Sequence: | 193540150 | Sequence: | 193540151 | Sequence: | 193540152 | Sequence: | 193540153 |
Mesh Term | Hemorrhoids | Mesh Term | Pain, Procedural | Mesh Term | Rectal Diseases | Mesh Term | Intestinal Diseases | Mesh Term | Gastrointestinal Diseases | Mesh Term | Digestive System Diseases | Mesh Term | Vascular Diseases | Mesh Term | Cardiovascular Diseases | Mesh Term | Pain | Mesh Term | Neurologic Manifestations |
Downcase Mesh Term | hemorrhoids | Downcase Mesh Term | pain, procedural | Downcase Mesh Term | rectal diseases | Downcase Mesh Term | intestinal diseases | Downcase Mesh Term | gastrointestinal diseases | Downcase Mesh Term | digestive system diseases | Downcase Mesh Term | vascular diseases | Downcase Mesh Term | cardiovascular diseases | Downcase Mesh Term | pain | Downcase Mesh Term | neurologic manifestations |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48332338 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Advocate Health Care |
Design Group Interventions
Sequence: | 68168185 |
Design Group Id | 55609122 |
Intervention Id | 52499435 |
Eligibilities
Sequence: | 30773579 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
Patients older than 18 years of age Exclusion Criteria: Patients undergoing endoscopic hemorrhoids band ligation who are already on pain medications chronically due to other reasons |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253952727 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2018 |
Actual Duration | 18 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | True |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 1 |
Designs
Sequence: | 30519710 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Supportive Care |
Time Perspective | |
Masking | Triple |
Subject Masked | True |
Caregiver Masked | True |
Outcomes Assessor Masked | True |
Responsible Parties
Sequence: | 28886011 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797690
2020-11-02
https://zephyrnet.com/?p=NCT03797690
NCT03797690https://www.clinicaltrials.gov/study/NCT03797690?tab=tableJohann BEAUDREUIL, PUPHjohann.beaudruil@aphp.fr+33 1 49 95 88 28The main objective is to investigate if percutaneous needle aponeurotomy is non-inferior to open surgery using aponeurectomy in treatment of flexion contracture due to Dupuytren’s disease.
Our hypothesis is that percutaneous needle aponeurotomy has suitable efficacy and safety profile for large application in the treatment of Dupuytren’s disease and that it is consequently able to drastically reduce the need of open surgery in this indication.
<![CDATA[
Studies
Study First Submitted Date | 2018-06-25 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2022-12-08 |
Start Month Year | November 2, 2020 |
Primary Completion Month Year | March 14, 2025 |
Verification Month Year | November 2022 |
Verification Date | 2022-11-30 |
Last Update Posted Date | 2022-12-08 |
Detailed Descriptions
Sequence: | 20663965 |
Description | Scientific justification:
Dupuytren's disease is a world-wide musculoskeletal disorder. It consists in fibrosis of the palmar aponeurosis that can induce disabling flexion contracture of the metacarpophalageal or proximal interphalangeal joints. Treatment modalities of flexion contracture include open surgery, percutaneous needle aponeurotomy and collagenase. Collagenase is not available in France. Aponeurectomy, that is also called fasciectomy, is the main open surgical technique, and open surgery is the most frequently used treatment in Dupuytren's disease. Percutaneous needle aponeurotomy is recommended as a nonsurgical treatment for Dupuytren's disease. It is a minimally invasive procedure. Its most largely accepted indication is Dupuytren's disease with metacarpophalageal joint involvement. However, percutaneous needle aponeurotomy has been successful for metacarpophalageal or proximal interphalangeal joint involvement, in nonadvanced and in advanced Dupuytren's disease. A model analysis recently demonstrated that replacing open surgery with percutaneous needle aponeurotomy could save more than 50% of the total hospitalization costs for the disease. Percutaneous needle aponeurotomy therefore appears as a unique minimally invasive approach for Dupuytren's disease. It could become a valuable alternative to open surgery. The hypothesis is that percutaneous needle aponeurotomy has suitable efficacy and safety profile for large application in the treatment of Dupuytren's disease and that it is consequently able to drastically reduce the need of open surgery in this indication. Practical procedure: Patients addressed to the consultation of the hand surgery centers for Dupuytren's disease will be prospectively selected, included, randomized, treated using percutaneous needle aponeurotomy or open surgery within six weeks after randomization, and followed at 1 week, 1, 3,12, 24 and 36 months after treatment. Assessment of efficacy will be blinded. Assessment of complications will be done by an unblinded assessor. |
Facilities
Sequence: | 199452811 | Sequence: | 199452812 | Sequence: | 199452813 | Sequence: | 199452814 |
Status | Active, not recruiting | Status | Active, not recruiting | Status | Recruiting | Status | Recruiting |
Name | Centre d'Imagerie Médicale Bachaumont Paris Centre | Name | Hopital LARIBOISIERE – Radiologie | Name | Hopital LARIBOISIERE – Rhumatologie | Name | JOUVENET – Orthopédie, chirurgie de la main et du membre supérieur |
City | Paris | City | Paris | City | Paris | City | Paris |
Zip | 75002 | Zip | 75010 | Zip | 75010 | Zip | 75016 |
Country | France | Country | France | Country | France | Country | France |
Facility Contacts
Sequence: | 28030496 | Sequence: | 28030497 |
Facility Id | 199452813 | Facility Id | 199452814 |
Contact Type | primary | Contact Type | primary |
Name | Johann BEAUDREUIL, PUPH | Name | ERIC ROULOT, PH |
johann.beaudreuil@aphp.fr | secretaire.roulot@gmail.com | ||
Phone | 01 49 95 88 28 | Phone | 01 42 15 42 33 |
Conditions
Sequence: | 52020500 |
Name | Dupuytren Disease of Finger |
Downcase Name | dupuytren disease of finger |
Id Information
Sequence: | 40040581 |
Id Source | org_study_id |
Id Value | P160903J |
Countries
Sequence: | 42437035 |
Name | France |
Removed | False |
Design Groups
Sequence: | 55427655 | Sequence: | 55427656 |
Group Type | Experimental | Group Type | Active Comparator |
Title | Percutaneous needle aponeurotomy | Title | Open surgery with limited aponeurectomy |
Description | It consists in cutting the fibrotic cord due to the disease and responsible for the flexion contracture, with a needle under local anesthesia. The procedure can be repeated as required during the same session. One to three sessions with at least one-week interval are usually sufficient and will be allowed. It will be performed in outpatient setting by a senior physician experienced in the procedure. End of treatment will be considered as the last session of needle aponeurotomy. | Description | It consists in excision of the fibrotic aponeurosis.It will be performed by hand surgeons under loco-regional anaesthesia during a short hospitalization (1 day stay). Post-operative cares are necessary (analgesics, splint, nursing, physiotherapy). End of surgical treatment will be considered as the removal of the stitches (two weeks after the surgical treatment). |
Interventions
Sequence: | 52333132 | Sequence: | 52333133 |
Intervention Type | Procedure | Intervention Type | Procedure |
Name | Percutaneous needle aponeurotomy | Name | Open surgery with limited aponeurectomy |
Description | It consists in cutting the fibrotic cord due to the disease and responsible for the flexion contracture, with a needle under local anesthesia. The procedure can be repeated as required during the same session. One to three sessions with at least one-week interval are usually sufficient and will be allowed. It will be performed in outpatient setting by a senior physician experienced in the procedure | Description | It consists in excision of the fibrotic aponeurosis.It will be performed by hand surgeons under loco-regional anaesthesia during a short hospitalization (1 day stay). Post-operative cares are necessary (analgesics, splint, nursing, physiotherapy) |
Keywords
Sequence: | 79626289 | Sequence: | 79626290 | Sequence: | 79626291 | Sequence: | 79626292 |
Name | Dupuytren's disease | Name | Percutaneous needle aponeurotomy | Name | Limited aponeurectomy | Name | Randomized trial |
Downcase Name | dupuytren's disease | Downcase Name | percutaneous needle aponeurotomy | Downcase Name | limited aponeurectomy | Downcase Name | randomized trial |
Design Outcomes
Sequence: | 176855118 | Sequence: | 176855119 | Sequence: | 176855120 | Sequence: | 176855121 | Sequence: | 176855122 | Sequence: | 176855123 | Sequence: | 176855124 | Sequence: | 176855125 | Sequence: | 176855126 | Sequence: | 176855127 | Sequence: | 176855128 | Sequence: | 176855129 | Sequence: | 176855130 | Sequence: | 176855131 | Sequence: | 176855132 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Metacarpophalangeal joint contracture during passive extension | Measure | Metacarpophalangeal joint contractures during passive and active extension | Measure | Main metacarpophalangeal joint contracture during passive extension, | Measure | The clinical success | Measure | The recurrence | Measure | The interphalangeal joint contractures during passive and active extension | Measure | The 70% improvement from baseline of the flexion contracture | Measure | The active range of motion of metacarpophalangeal and proximal interphalangeal treated joints | Measure | The functional limitation using Quick DASH questionnaire | Measure | The URAM scale | Measure | The patient satisfaction on a 0-100 mm visual analog scale | Measure | The number of secondary and repeated treatments | Measure | Complications and adverse events for primary treatment | Measure | Complications and adverse events for secondary treatment | Measure | The post-interventional pain and needs |
Time Frame | at 3 months after treatment | Time Frame | at 1 week, 1, 3, 12, 24 and 36 months after treatment | Time Frame | at 36 months after treament | Time Frame | at 3 months after treament | Time Frame | at 12, 24 and 36 months after treament | Time Frame | at 1 week, 1, 3,12, 24 and 36 months after treatment | Time Frame | at 1 week, 1, 3, 12, 24 and 36 months after treatment | Time Frame | at 1 week, 1, 3, 12, 24 and 36 months after treatment | Time Frame | at 1 week, 1, 3, 12, 24 and 36 months after treatment | Time Frame | at 1 week, 1, 3, 12, 24 and 36 months after treatment | Time Frame | at 1 week, 1, 3, 12, 24 and 36 months after treatment | Time Frame | at 12, 24 and 36 months after treatment | Time Frame | at the treatment time, and at 1 week, 1, 3, 12, 24 and 36 months; | Time Frame | at the treatment time, at 12, 24 and 36 months; | Time Frame | at 1 week, 1, 3, 12, 24 and 36 months |
Description | Expressed in degrees, using low energy computed tomography for blinded assessment (computed tomography imaging will be analysed by a blinded assessor not involved in the treatment). Baseline will be Metacarpophalangeal joint contracture during passive extension the day of the treatment, before any treatment | Description | Expressed in degrees using clinical goniometry, and patient wearing white opac gloves to ensure blinded assessment. | Description | Expressed in degrees, using low energy computed tomography, for blinded assessment (computed tomography imaging will be analysed by a blinded assessor not involved in the treatment). | Description | The clinical success is defined as the reduction of flexum to within 0 to 5° during passive extension, using clinical goniometry, for the main metacarpophalangeal joint); Patient will wear white opac gloves to ensure blinded assessment. | Description | The recurrence is defined as the flexum progression of 20°, during passive extension, using clinical goniometry, after clinical success. Patient will wear white opac gloves to ensure blinded assessment. | Description | Expressed in degrees, using clinical goniometry. Patient will wear white opac gloves to ensure blinded assessment. | Description | The flexion contracture of each treated joint, during passive extension will be assessed by a blinded assessor (Patient will wear white opac gloves). – Flexion contracture in degrees using goniometry reported as follows: ray Number; metacarpophalangeal angle; interphalangeal angle | Description | The active range of motion of metacarpophalangeal and proximal interphalangeal treated joints will be assessed by a blinded assessor (Patient will wear white opac gloves). | Description | The patient will fill out the auto-questionnaire. The blinded assessor will calculate the score (0 to 100, with highest value indicating highest disability). | Description | The patient will fill out the auto-questionnaire. The blinded assessor will calculate the score (0 to 45, with highest value indicating highest disability). | Description | The assessor will ask the patient the following question: "How would you rate satisfaction about the treatment you underwent in the study?" Patients will be asked to mark the level of their satisfaction on a l00-mm, nonhatched VAS scale marked at one end as "not satisfied" and at the other as "completely satisfied'' | Description | The number of secondary or repeated open surgeries and percutaneous needle aponeurotomy will be recorded by the unblinded assessor. | Description | The number and the types of complications and adverse events for primary open surgery and first line percutaneous needle aponeurotomy will be collected by an unblinded assessor. | Description | The number and the types of complications and adverse events for secondary open surgery and percutaneous needle aponeurotomy will be collected by an unblinded assessor. | Description | The post-interventional pain and needs of nursing, splinting, medication, physiotherapy,sick leave, time return to regular activities using a patient diary. These datas will be collected by the unblinded assessor. |
Browse Conditions
Sequence: | 192889470 | Sequence: | 192889471 | Sequence: | 192889472 | Sequence: | 192889473 | Sequence: | 192889474 | Sequence: | 192889475 | Sequence: | 192889476 | Sequence: | 192889477 | Sequence: | 192889478 | Sequence: | 192889479 | Sequence: | 192889480 |
Mesh Term | Dupuytren Contracture | Mesh Term | Fibroma | Mesh Term | Neoplasms, Fibrous Tissue | Mesh Term | Neoplasms, Connective Tissue | Mesh Term | Neoplasms, Connective and Soft Tissue | Mesh Term | Neoplasms by Histologic Type | Mesh Term | Neoplasms | Mesh Term | Contracture | Mesh Term | Muscular Diseases | Mesh Term | Musculoskeletal Diseases | Mesh Term | Connective Tissue Diseases |
Downcase Mesh Term | dupuytren contracture | Downcase Mesh Term | fibroma | Downcase Mesh Term | neoplasms, fibrous tissue | Downcase Mesh Term | neoplasms, connective tissue | Downcase Mesh Term | neoplasms, connective and soft tissue | Downcase Mesh Term | neoplasms by histologic type | Downcase Mesh Term | neoplasms | Downcase Mesh Term | contracture | Downcase Mesh Term | muscular diseases | Downcase Mesh Term | musculoskeletal diseases | Downcase Mesh Term | connective tissue diseases |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48178859 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Assistance Publique – Hôpitaux de Paris |
Overall Officials
Sequence: | 29198734 |
Role | Principal Investigator |
Name | Johann BEAUDREUIL, PUPH |
Affiliation | APHP |
Central Contacts
Sequence: | 11975275 |
Contact Type | primary |
Name | Johann BEAUDREUIL, PUPH |
Phone | +33 1 49 95 88 28 |
johann.beaudruil@aphp.fr | |
Role | Contact |
Design Group Interventions
Sequence: | 67948321 | Sequence: | 67948322 |
Design Group Id | 55427655 | Design Group Id | 55427656 |
Intervention Id | 52333132 | Intervention Id | 52333133 |
Eligibilities
Sequence: | 30677198 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Age ≥ 18 years old Exclusion Criteria: Presence of other musculoskeletal disorders of the hand than Dupuytren's disease: known inflammatory rheumatic disease of the hand, clinical signs of inflammatory rheumatic disease of the hand, MP or PIP pain at inclusion visit. |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253870611 |
Number Of Facilities | 4 |
Registered In Calendar Year | 2018 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | False |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 14 |
Designs
Sequence: | 30423951 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Double |
Masking Description | The primary outcome (main metacarpophalangeal joint contracture during passive extension) will be assessed using low energy computed tomography before treatment, 3 months and 36 months after treatment for blinded assessment. Furthermore, in addition to the clinical follow-up, the patient will be followed by a blinded assessor. At each follow-up visits with the blinded assessor, patient will be asked to wear white opaque gloves to ensure the blinding for the treatment during assessment including the main outcome. Clinicians, nurses and patients will be instructed to the importance of avoiding communication about the treatment to the blinded assessor. |
Intervention Model Description | multicenter, non-inferiority PROBE (Prospective Randomized Open Blinded End-point) trial. Two groups (ratio 1:1) will be compared in this phase III pivotal study: experimental group versus control group. |
Investigator Masked | True |
Outcomes Assessor Masked | True |
Responsible Parties
Sequence: | 28790471 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797677
2017-03-09
https://zephyrnet.com/?p=NCT03797677
NCT03797677https://www.clinicaltrials.gov/study/NCT03797677?tab=tableNANANAThe study was a non-randomized open label pilot study. It was an observational design conducted at one (1) site in the US. All enrolled subjects received treatment with the MN4000.
This pilot study evaluated subject satisfaction with the therapy and adherence to the therapy during the 90-day treatment period, and also collected clinical outcome data. Outcomes were assessed before, during and after the MN4000 treatment period.
<![CDATA[
Studies
Study First Submitted Date | 2018-12-27 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-09 |
Start Month Year | March 9, 2017 |
Primary Completion Month Year | November 30, 2017 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-09 |
Detailed Descriptions
Sequence: | 20735940 |
Description | The study was a non-randomized open label pilot study. It was an observational design conducted at one (1) site in the US. All enrolled subjects received treatment with the MN4000.
This pilot study evaluated subject satisfaction with the therapy and adherence to the therapy during the 90-day treatment period, and also collected clinical outcome data. Outcomes were assessed before, during and after the MN4000 treatment period. The study did not include a control group. This pilot study was designed to provide initial information that could inform decisions for future larger-scale studies. Ten (10) patients total were enrolled from CF and NMD clinics. Eligible subjects were adult patients who were able to perform MN4000 therapy using a mouthpiece and who met all inclusion and none of the exclusion criteria. All patients received therapy with the MN4000 following the labeled instructions for the device. The MN4000 is an airway clearance and lung expansion therapy device that has been cleared to market by the FDA as The MetaNeb® System for Homecare environment, for clearance of pulmonary secretions and for treatment or prevention of pulmonary atelectasis. It is a Class II device, cleared to market on March 17, 2016 under premarket notification 510(k) K151689 as The MetaNeb® 4 System with application for homecare environment. It is commercially marketed as the MN4000. The device consists of a pneumatic compressor and an air pulse generator that delivers CHFO and CPEP to; facilitate clearance of mucous from the lungs; This "triple" mode device can provide aerosol therapy while alternating between CPEP for lung expansion and CHFO for airway clearance. Supplemental oxygen therapy may also be delivered when used with compressed oxygen. The MN4000 has three therapy modes: CHFO (Continuous High Frequency Oscillation) – delivers aerosol therapy while providing oscillating pressure pulses to the airway After assessing baseline status, therapy with the MN4000 was introduced and incorporated into the daily home respiratory care treatment regimen for all patients. Other airway clearance and/or lung expansion therapies were not to be performed during the three-month study period. The treatment regimen for other respiratory care modalities (e.g. aerosolized medications) was that which was prescribed by the patient's health care team in the routine standard care of each patient. During the three-month follow-up period, adherence to the daily prescribed therapy regimen was assessed. Subjects/caregivers were asked to provide adherence information for each day during the 90-day study period. Documentation of efficacy and safety Variables was completed by study staff at the time of occurrence, from review of the patient's medical records and from scores and rankings for questionnaires. |
Facilities
Sequence: | 200245068 |
Name | Northwestern |
City | Chicago |
State | Illinois |
Zip | 60208 |
Country | United States |
Conditions
Sequence: | 52208492 | Sequence: | 52208493 | Sequence: | 52208494 |
Name | Cystic Fibrosis | Name | Motor Neuron Disease | Name | Airway Clearance Impairment |
Downcase Name | cystic fibrosis | Downcase Name | motor neuron disease | Downcase Name | airway clearance impairment |
Id Information
Sequence: | 40186439 |
Id Source | org_study_id |
Id Value | CR-RR2016-002 |
Countries
Sequence: | 42599934 |
Name | United States |
Removed | False |
Design Groups
Sequence: | 55635115 |
Group Type | Experimental |
Title | Home based airway clearance with Metaneb |
Description | Patients with CF and MND who required regular home airway clearance therapy were enrolled to use the Metaneb device in the home setting.
The MN4000 is an airway clearance and lung expansion therapy device that has been cleared to market by the FDA as The MetaNeb® System for Homecare environment, for clearance of pulmonary secretions and for treatment or prevention of pulmonary atelectasis. It is a Class II device, cleared to market on March 17, 2016 under premarket notification 510(k) K151689 as The MetaNeb® 4 System with application for homecare environment. |
Interventions
Sequence: | 52522459 |
Intervention Type | Device |
Name | MN 4000 |
Description | Patients who required regular home airway clearance therapy were enrolled in the study and were prescribed therapy with the MN4000. Adherence to the prescribed therapy regimen and patient/caregiver satisfaction with the therapy was assessed. Pulmonary function, was assessed for each subject at baseline, after 1 month and after 3 months of home therapy. Results from the therapy period was compared to the baseline period, during which the subject received their regular airway clearance regimen. Airway Clearance Satisfaction surveys were conducted at baseline, after 1 month, and after 3 months of therapy. Results from the MN4000 therapy period were compared to the baseline period, during which the subject received their regular regimen |
Keywords
Sequence: | 79923525 | Sequence: | 79923526 | Sequence: | 79923527 | Sequence: | 79923528 |
Name | Airway Clearance | Name | Cystic Fibrosis | Name | Motor Neuron Disease | Name | Home care |
Downcase Name | airway clearance | Downcase Name | cystic fibrosis | Downcase Name | motor neuron disease | Downcase Name | home care |
Design Outcomes
Sequence: | 177512730 | Sequence: | 177512731 | Sequence: | 177512732 | Sequence: | 177512733 | Sequence: | 177512734 | Sequence: | 177512735 | Sequence: | 177512736 | Sequence: | 177512737 | Sequence: | 177512738 | Sequence: | 177512739 | Sequence: | 177512740 | Sequence: | 177512741 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Patient / Caregiver Satisfaction scores | Measure | Mean adherence to prescribed treatment regimen | Measure | ALS-Functional Rating Scale (ALS-FRS) | Measure | Cystic Fibrosis Questionnaire – Revised (CFQ-R) | Measure | Exacerbation of pulmonary disease | Measure | FEV1 | Measure | FVC | Measure | FEV1/FVC ratio | Measure | SVC | Measure | SPO2 | Measure | Maximal inspiratory pressure (MIP) | Measure | PCF |
Time Frame | 90 days | Time Frame | 90 days | Time Frame | 90 days | Time Frame | 90 days | Time Frame | 90 days | Time Frame | 90 days | Time Frame | 90 days | Time Frame | 90 days | Time Frame | 90 days | Time Frame | 90 days | Time Frame | 90 days | Time Frame | 90 days |
Description | The primary efficacy variable was patient and/or caregiver satisfaction with therapy, as evaluated using a Therapy Use Rating Scale questionnaire. The Therapy Use Rating Scale is an assessment of patient/caregiver satisfaction with the therapy and their subjective assessment of the benefit of the therapy. This was assessed by a 5 point likert scale assessing effectiveness, ease of use and likelihood to continue therapy with 5 representing positive responses and 1, negative. | Description | Evidenced by feedback on adherence to therapy. Use of the MN4000 was evaluated, collecting daily treatment usage information from study subjects and/or caregivers to determine the level of adherence to the prescribed therapy regimen. A self reporting tool has been developed for the study assessing adherence to duration of individual prescribed treatment time and overall study duration. | Description | MND patients only. MND patients only. The Amyotrophic Lateral Sclerosis Functional Rating Scale (ALSFRS) is an instrument for evaluating the functional status of patients with Amyotrophic Lateral Sclerosis. It can be used to monitor functional change in a patient over time.
It contains 10 distinct measures: Speech These 10 parameters are scored on a scale of 0-4, based on the patients' ability to perform tasks. The minimum score is 0 and maximum 40.The higher the score the more function is retained. |
Description | CF patients only. The Cystic Fibrosis Questionnaire (CFQ) is a disease-specific instrument that measures health-related quality of life (HRQOL) for adolescents and adults with cystic fibrosis (CF) > or = 14 years, consisting of 44 items on 12 generic and disease-specific scales. It offers 5 distinct 4-point Likert scales (e.g., always/often/ sometime/never). Scores for each HRQoL domain; after recoding, each item is summed to generate a domain score and standardized. Scores range from 0 to 100, with higher scores indicating better health. | Description | Hospitalization and/or antibiotics for respiratory infection or complication. Exacerbations of pulmonary disease were defined as respiratory infections that resulted in requirement for hospitalization and/or antibiotics to treat the respiratory infection or complication. Hospitalizations that are part of routine care (e.g. hospital admissions for annual "tune-up") or antibiotics that are part of the regular treatment regimen were not documented as exacerbations. Occurence of exarcerbation related hospitalization OR the necessity of a prescription for antibiotics qualify as worsening disease. | Description | FEV1: The forced expiratory volume-one second is the total volume of air a patient exhales in the first second during maximal effort. Normal range is >80%. Decreasing percentage is associated with worsening / Severe disease | Description | The functional vital capacity is the total volume of air a patient exhales for the total duration of the test during maximal effort. Normal range is >80%. Decreasing percentage is associated with worsening / Severe disease | Description | The percentage of the FVC expired in one second Results are given in both raw data (litres, litres per second) and % predicted-the test result as a percent of the "predicted values" for the patients of similar characteristics. Results over 80% are considered normal. | Description | Slow Vital Capacity displays the volume of gas measured on a complete expiration after a maximal inspiration without forced or rapid effort. Useful measurement when FVC is reduced and airway obstruction is present. educed SVC is associated with worsening respiratory disease | Description | SpO2 stands for peripheral capillary oxygen saturation, an estimate of the amount of oxygen in the blood. Low SPO2 is associated with worsening respiratory function. | Description | Maximal inspiratory pressure (MIP) is a measure of the strength of inspiratory muscles, primarily the diaphragm, and allows for the assessment of ventilatory failure, restrictive lung disease and respiratory muscle strength. Reduction in MIP is asociated with worsening neuromuscular status and poor ability to cough. | Description | The Peak Cough Flow is the maximum air flow generated during a cough. Decreasing air flow generated is associated with weakening neuromuscular status and associated poor cough impulse |
Browse Conditions
Sequence: | 193628556 | Sequence: | 193628557 | Sequence: | 193628558 | Sequence: | 193628559 | Sequence: | 193628561 | Sequence: | 193628562 | Sequence: | 193628563 | Sequence: | 193628564 | Sequence: | 193628565 | Sequence: | 193628566 | Sequence: | 193628567 | Sequence: | 193628568 | Sequence: | 193628569 | Sequence: | 193628570 | Sequence: | 193628571 | Sequence: | 193628572 | Sequence: | 193628573 | Sequence: | 193628574 | Sequence: | 193628560 |
Mesh Term | Cystic Fibrosis | Mesh Term | Motor Neuron Disease | Mesh Term | Amyotrophic Lateral Sclerosis | Mesh Term | Fibrosis | Mesh Term | Pancreatic Diseases | Mesh Term | Digestive System Diseases | Mesh Term | Lung Diseases | Mesh Term | Respiratory Tract Diseases | Mesh Term | Genetic Diseases, Inborn | Mesh Term | Infant, Newborn, Diseases | Mesh Term | Neurodegenerative Diseases | Mesh Term | Nervous System Diseases | Mesh Term | Neuromuscular Diseases | Mesh Term | Spinal Cord Diseases | Mesh Term | Central Nervous System Diseases | Mesh Term | TDP-43 Proteinopathies | Mesh Term | Proteostasis Deficiencies | Mesh Term | Metabolic Diseases | Mesh Term | Pathologic Processes |
Downcase Mesh Term | cystic fibrosis | Downcase Mesh Term | motor neuron disease | Downcase Mesh Term | amyotrophic lateral sclerosis | Downcase Mesh Term | fibrosis | Downcase Mesh Term | pancreatic diseases | Downcase Mesh Term | digestive system diseases | Downcase Mesh Term | lung diseases | Downcase Mesh Term | respiratory tract diseases | Downcase Mesh Term | genetic diseases, inborn | Downcase Mesh Term | infant, newborn, diseases | Downcase Mesh Term | neurodegenerative diseases | Downcase Mesh Term | nervous system diseases | Downcase Mesh Term | neuromuscular diseases | Downcase Mesh Term | spinal cord diseases | Downcase Mesh Term | central nervous system diseases | Downcase Mesh Term | tdp-43 proteinopathies | Downcase Mesh Term | proteostasis deficiencies | Downcase Mesh Term | metabolic diseases | Downcase Mesh Term | pathologic processes |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48354112 |
Agency Class | INDUSTRY |
Lead Or Collaborator | lead |
Name | Hill-Rom |
Overall Officials
Sequence: | 29306197 |
Role | Principal Investigator |
Name | Lisa F Wolfe, MD |
Affiliation | Northwestern University |
Design Group Interventions
Sequence: | 68199719 |
Design Group Id | 55635115 |
Intervention Id | 52522459 |
Eligibilities
Sequence: | 30787106 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Documented diagnosis of CF or MND Exclusion Criteria: Requirement for continuous mechanical ventilation |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253990028 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2018 |
Actual Duration | 8 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | True |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 11 |
Designs
Sequence: | 30533176 |
Allocation | N/A |
Intervention Model | Single Group Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | None (Open Label) |
Provided Documents
Sequence: | 2582508 |
Document Type | Study Protocol and Statistical Analysis Plan |
Has Protocol | True |
Has Icf | False |
Has Sap | True |
Document Date | 2016-12-05 |
Url | https://ClinicalTrials.gov/ProvidedDocs/77/NCT03797677/Prot_SAP_000.pdf |
Responsible Parties
Sequence: | 28899469 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797664
2018-12-14
https://zephyrnet.com/?p=NCT03797664
NCT03797664https://www.clinicaltrials.gov/study/NCT03797664?tab=tableNANANAThe purpose of this study is to assess the safety and tolerability of an oral solution of CDX-6114 when administered as a single dose in healthy volunteers
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2021-08-04 |
Start Month Year | December 14, 2018 |
Primary Completion Month Year | April 12, 2019 |
Verification Month Year | August 2021 |
Verification Date | 2021-08-31 |
Last Update Posted Date | 2021-08-04 |
Detailed Descriptions
Sequence: | 20721680 |
Description | This is a second Phase 1, double-blind, placebo-controlled study in approximately 24 healthy volunteers who are 18 to 55 years old. Three cohorts are planned each consisting of 8 subjects; the cohorts as planned are 7.5, 15.0 and 22.5 g of CDX-6114 (or matching placebo) in oral solution. Increasing doses of CDX-6114 will be assessed sequentially un til the final dose is evaluated or any of the stopping criteria are reached. Subjects will each receive either a single dose of CDX-6114 or matching placebo, with food, and will then be followed for a total of 22 days (3 weeks). |
Facilities
Sequence: | 200108802 |
Name | Linear Clinical Services |
City | Perth |
State | Western Australia |
Zip | 6009 |
Country | Australia |
Conditions
Sequence: | 52171369 |
Name | Healthy |
Downcase Name | healthy |
Id Information
Sequence: | 40158708 |
Id Source | org_study_id |
Id Value | CDX6114-004 |
Countries
Sequence: | 42569044 |
Name | Australia |
Removed | False |
Design Groups
Sequence: | 55593297 | Sequence: | 55593298 |
Group Type | Experimental | Group Type | Placebo Comparator |
Title | Experimental: CDX-6114 | Title | Placebo Comparator: Placebo |
Description | 7.5, 15.0 and 22.5g | Description | Phosphate Buffer Diluent Solution |
Interventions
Sequence: | 52485591 | Sequence: | 52485592 |
Intervention Type | Drug | Intervention Type | Drug |
Name | CDX-6114 | Name | Placebo |
Description | CDX-6114 will be administered as a single, oral dose solution at dose levels of 7.5, 15.0 and 22.5g | Description | Phosphate Buffer Diluent oral solution |
Design Outcomes
Sequence: | 177379272 | Sequence: | 177379273 | Sequence: | 177379274 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary |
Measure | The incidence of treatment-emergent adverse events experienced by the subjects following oral administration of CDX-6114 | Measure | Pharmacokinetics of CDX-6114 | Measure | Pharmacodynamics of CDX-6114 |
Time Frame | Up to 22 days after drug administartion | Time Frame | Up to 24 hours after drug administration | Time Frame | Up to 24 hours after drug administration |
Description | Will be measured by assessing the frequency and the nature of the AEs reported | Description | Assessed by the serum levels of CDX-6114 following oral administration of CDX-6114 | Description | Assessed by the plasma levels of phenylalanine and cinnamic acid following oral administration of CDX-6114 |
Sponsors
Sequence: | 48319403 |
Agency Class | INDUSTRY |
Lead Or Collaborator | lead |
Name | Codexis Inc. |
Overall Officials
Sequence: | 29285411 |
Role | Principal Investigator |
Name | Sam Salman |
Affiliation | Linear Clinical Services |
Design Group Interventions
Sequence: | 68149269 | Sequence: | 68149270 |
Design Group Id | 55593297 | Design Group Id | 55593298 |
Intervention Id | 52485591 | Intervention Id | 52485592 |
Eligibilities
Sequence: | 30765417 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 55 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
Healthy male and female, non-smoking, subjects between the ages of 18 and 55 years, inclusive, at the time of screening. Male subjects and their female spouse/partner(s) who are of childbearing potential: Must agree to stay abstinent (where abstinence is the preferred and usual life-style of the subject), starting at screening and continuing throughout the clinical study period, and for 90 days after study drug administration. Or Must be using highly effective contraception consisting of 2 forms of birth control (1 of which must be a barrier method) starting at screening and continuing throughout the clinical study period, and for 90 days after study drug administration. Female subjects of childbearing potential: Must agree not to become pregnant during the clinical study period and for 30 days after study drug administration. If heterosexually active, must agree to consistently use a form of highly effective birth control, in combination with a barrier method starting at screening and continuing throughout the clinical study period, and for 30 days after study drug administration Or Must agree to stay abstinent, (where abstinence is the preferred and usual life-style of the subject), starting at screening and continuing throughout the clinical study period, and for 30 days after study drug administration. Female subjects of non-childbearing potential: Must have a confirmed clinical history of sterility Or Must be postmenopausal as defined as: amenorrhea for at least 1 year prior to screening and a laboratory confirmed serum follicle stimulating hormone (FSH) level ≥ 40mIU/mL. Subject agrees not to participate in another interventional study while participating in the present clinical study. – Exclusion Criteria: Female subject who has been pregnant within the 6 months prior to screening or breastfeeding within the 3 months prior to screening. Known allergy or adverse reaction history to any of the oral dose formulation components e.g. mannitol – |
Adult | True |
Child | False |
Older Adult | False |
Calculated Values
Sequence: | 253889233 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Actual Duration | 3 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 55 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 2 |
Designs
Sequence: | 30511583 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Quadruple |
Masking Description | Double-Blind |
Intervention Model Description | Dose-escalating, Randomized, Double-Blinded,. Placebo-Controlled |
Subject Masked | True |
Caregiver Masked | True |
Investigator Masked | True |
Outcomes Assessor Masked | True |
Responsible Parties
Sequence: | 28877878 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797651
2019-04-24
https://zephyrnet.com/?p=NCT03797651
NCT03797651https://www.clinicaltrials.gov/study/NCT03797651?tab=tableMyeong-Ki Hong, MD, PhDmkhong61@yuhs.ac82-2-2228-8458We hypothesized that ticagrelor monotherapy might be enough to prevent thromboembolic events without aspirin after PCI in patients with acute coronary syndrome(ACS). Moreover, ticagrelor monotherapy will reduce bleeding risk compared to DAPT with aspirin plus ticagrelor. We will also evaluate 1-year safety and efficacy of Orsiro stent for patient with acute coronary syndrome. After confirmation of enrollment, patients will be randomized to continue standard treatment (aspirin plus ticagrelor) for 1 year or to stop aspirin after discharge or less than 1 month after PCI (ticagrelor monotherapy). Randomization will be stratified according to 1) the presence of diabetes and 2) ST elevation myocardial infarction (MI). Baseline clinical and angiographic characteristics, laboratory findings will be assessed at the time of randomization. All patients will provide informed consent on their own initiative.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-06 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2023-03-07 |
Start Month Year | April 24, 2019 |
Primary Completion Month Year | April 4, 2025 |
Verification Month Year | March 2023 |
Verification Date | 2023-03-31 |
Last Update Posted Date | 2023-03-07 |
Facilities
Sequence: | 199785018 |
Status | Recruiting |
Name | Yonsei Cardiovascular Center and Cardiovascular Research Institute, Yonsei University College of Medicine |
City | Seoul |
Zip | 03722 |
Country | Korea, Republic of |
Facility Contacts
Sequence: | 28075000 |
Facility Id | 199785018 |
Contact Type | primary |
Name | Myeong-Ki Hong, MD, PhD |
mkhong61@yuhs.ac | |
Phone | 82-2-2228-8458 |
Conditions
Sequence: | 52104184 |
Name | Coronary Artery Disease, Acute Coronary Syndrome |
Downcase Name | coronary artery disease, acute coronary syndrome |
Id Information
Sequence: | 40106111 |
Id Source | org_study_id |
Id Value | 4-2018-0782 |
Countries
Sequence: | 42508632 |
Name | Korea, Republic of |
Removed | False |
Design Groups
Sequence: | 55520476 | Sequence: | 55520477 |
Group Type | Active Comparator | Group Type | Experimental |
Title | Standard DAPT | Title | Very-short DAPT within 1 month |
Description | Patient will continue standard treatment (aspirin plus ticagrelor) for 1 year. Dosage of ticagrelor would be 90 mg twice a day, and 100 mg of aspirin will be prescribed once a day. | Description | Patient will stop aspirin after discharge (DAPT less than 1 months after PCI) (ticagrelor monotherapy). Dosage of ticagrelor would be 90 mg twice a day, and 100 mg of aspirin will be prescribed once a day (during hospitalization). |
Interventions
Sequence: | 52418212 | Sequence: | 52418213 |
Intervention Type | Drug | Intervention Type | Drug |
Name | Standard DAPT | Name | Very-short DAPT less than 1 month after PCI |
Description | Patient will continue standard treatment (aspirin plus ticagrelor) for 1 year. Dosage of ticagrelor would be 90 mg twice a day, and 100 mg of aspirin will be prescribed once a day. | Description | Patient will stop aspirin (ticagrelor monotherapy) after discharge or within 1 month. Dosage of ticagrelor would be 90 mg twice a day, and 100 mg of aspirin will be prescribed once a day (during hospitalization). |
Design Outcomes
Sequence: | 177146235 | Sequence: | 177146236 | Sequence: | 177146237 | Sequence: | 177146238 | Sequence: | 177146239 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Net clinical benefit | Measure | Each components of net clinical benefit | Measure | Cardiovascular mortality | Measure | Major or minor bleeding | Measure | Major adverse cardiac event |
Time Frame | 1 year after procedure | Time Frame | 1 year after procedure | Time Frame | 1 year after procedure | Time Frame | 1 year after procedure | Time Frame | 1 year after procedure |
Description | A composite of all-cause death, MI, stent thrombosis, stroke, major bleeding | Description | All-cause death, MI, stent thrombosis, stroke, major bleeding | Description | Cardiovascular mortality | Description | Major or minor bleeding | Description | A composite of cardiac death, MI, stent thrombosis, ischemia-driven target-vessel revascularization |
Browse Conditions
Sequence: | 193223641 | Sequence: | 193223642 | Sequence: | 193223643 | Sequence: | 193223644 | Sequence: | 193223645 | Sequence: | 193223646 | Sequence: | 193223647 | Sequence: | 193223648 | Sequence: | 193223649 | Sequence: | 193223650 | Sequence: | 193223651 | Sequence: | 193223652 | Sequence: | 193223653 | Sequence: | 193223654 |
Mesh Term | Coronary Artery Disease | Mesh Term | Acute Coronary Syndrome | Mesh Term | Syndrome | Mesh Term | Acute Disease | Mesh Term | Disease | Mesh Term | Pathologic Processes | Mesh Term | Coronary Disease | Mesh Term | Myocardial Ischemia | Mesh Term | Heart Diseases | Mesh Term | Cardiovascular Diseases | Mesh Term | Arteriosclerosis | Mesh Term | Arterial Occlusive Diseases | Mesh Term | Vascular Diseases | Mesh Term | Disease Attributes |
Downcase Mesh Term | coronary artery disease | Downcase Mesh Term | acute coronary syndrome | Downcase Mesh Term | syndrome | Downcase Mesh Term | acute disease | Downcase Mesh Term | disease | Downcase Mesh Term | pathologic processes | Downcase Mesh Term | coronary disease | Downcase Mesh Term | myocardial ischemia | Downcase Mesh Term | heart diseases | Downcase Mesh Term | cardiovascular diseases | Downcase Mesh Term | arteriosclerosis | Downcase Mesh Term | arterial occlusive diseases | Downcase Mesh Term | vascular diseases | Downcase Mesh Term | disease attributes |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48257891 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Yonsei University |
Overall Officials
Sequence: | 29246925 |
Role | Principal Investigator |
Name | Myeong-Ki Hong |
Affiliation | Division of Cardiology, Severance Hospital, Yonsei University College of Medicine |
Central Contacts
Sequence: | 11994405 |
Contact Type | primary |
Name | Myeong-Ki Hong, MD, PhD |
Phone | 82-2-2228-8458 |
mkhong61@yuhs.ac | |
Role | Contact |
Design Group Interventions
Sequence: | 68059952 | Sequence: | 68059953 |
Design Group Id | 55520476 | Design Group Id | 55520477 |
Intervention Id | 52418212 | Intervention Id | 52418213 |
Eligibilities
Sequence: | 30727084 |
Gender | All |
Minimum Age | 19 Years |
Maximum Age | 80 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Patients ≥19 years old Exclusion Criteria: Age> 80 years |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253978812 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 19 |
Maximum Age Num | 80 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 4 |
Designs
Sequence: | 30473514 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | None (Open Label) |
Responsible Parties
Sequence: | 28839936 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797638
2018-10-01
https://zephyrnet.com/?p=NCT03797638
NCT03797638https://www.clinicaltrials.gov/study/NCT03797638?tab=tableNANANAWriter’s cramp is a focal dystonia characterized by abnormal movements and postures during writing. Limited finger independence during writing manifests as difficulty suppressing unwanted activations of neighbouring non task-relevant fingers. Patients with Writer’s cramp also have difficulty in fine control of grip force.
The investigators have recently developed the Finger Force Manipulandum which quantifies the forces applied by each fingers in different tasks. This method is sensitive for detection and quantification of small unwanted contractions in non-active (‘stationary’) fingers. Different tasks have been developed to assess abilities such as finger individuation but also fine finger force control, finger movement regularity and speed.
The aim of this study is to assess if developed tasks allow to precisely characterize writer’s cramp condition in terms of abilities aforementioned.
To do so, performance of 20 writer’s cramp patients in the developed task will be compared with performance of 20 control participants (matched in age, sex and writing hand) in the same tasks.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2021-06-22 |
Start Month Year | October 1, 2018 |
Primary Completion Month Year | July 19, 2019 |
Verification Month Year | June 2021 |
Verification Date | 2021-06-30 |
Last Update Posted Date | 2021-06-22 |
Facilities
Sequence: | 199965116 |
Name | Fondation A de Rothschild |
City | Paris |
Zip | 75019 |
Country | France |
Conditions
Sequence: | 52139058 | Sequence: | 52139059 | Sequence: | 52139060 |
Name | Dystonic Disorder | Name | Focal Dystonia | Name | Writer's Cramp |
Downcase Name | dystonic disorder | Downcase Name | focal dystonia | Downcase Name | writer's cramp |
Id Information
Sequence: | 40135103 |
Id Source | org_study_id |
Id Value | SSA_2018_4 |
Countries
Sequence: | 42542718 |
Name | France |
Removed | False |
Design Groups
Sequence: | 55559413 | Sequence: | 55559414 |
Group Type | Experimental | Group Type | Other |
Title | Patients with writer's cramp | Title | Control subjects |
Description | Patients with writer's cramp | Description | Control subjects, without writer's cramp, matched with case subjects with age, gender and hand writing |
Interventions
Sequence: | 52454969 |
Intervention Type | Device |
Name | Finger Force Manipuladum (FFM) |
Description | Tasks performed with the device Finger Force Manipuladum (FFM), to assess abilities such as finger individuation but also fine finger force control, finger movement regularity and speed. |
Keywords
Sequence: | 79822892 | Sequence: | 79822893 | Sequence: | 79822894 |
Name | Dystonic Disorder | Name | Focal Dystonia | Name | Writer's Cramp |
Downcase Name | dystonic disorder | Downcase Name | focal dystonia | Downcase Name | writer's cramp |
Design Outcomes
Sequence: | 177264037 |
Outcome Type | primary |
Measure | Manual dexterity by the FFM |
Time Frame | Inclusion |
Description | Compare the manual dexterity by the FFM between subjects with writer's cramp and control subject |
Browse Conditions
Sequence: | 193366748 | Sequence: | 193366749 | Sequence: | 193366750 | Sequence: | 193366751 | Sequence: | 193366752 | Sequence: | 193366753 | Sequence: | 193366742 | Sequence: | 193366743 | Sequence: | 193366744 | Sequence: | 193366745 | Sequence: | 193366746 | Sequence: | 193366747 |
Mesh Term | Nervous System Diseases | Mesh Term | Movement Disorders | Mesh Term | Central Nervous System Diseases | Mesh Term | Muscular Diseases | Mesh Term | Musculoskeletal Diseases | Mesh Term | Neuromuscular Manifestations | Mesh Term | Muscle Cramp | Mesh Term | Dystonia | Mesh Term | Dystonic Disorders | Mesh Term | Spasm | Mesh Term | Dyskinesias | Mesh Term | Neurologic Manifestations |
Downcase Mesh Term | nervous system diseases | Downcase Mesh Term | movement disorders | Downcase Mesh Term | central nervous system diseases | Downcase Mesh Term | muscular diseases | Downcase Mesh Term | musculoskeletal diseases | Downcase Mesh Term | neuromuscular manifestations | Downcase Mesh Term | muscle cramp | Downcase Mesh Term | dystonia | Downcase Mesh Term | dystonic disorders | Downcase Mesh Term | spasm | Downcase Mesh Term | dyskinesias | Downcase Mesh Term | neurologic manifestations |
Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48290756 | Sequence: | 48290757 |
Agency Class | NETWORK | Agency Class | OTHER_GOV |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator |
Name | Fondation Ophtalmologique Adolphe de Rothschild | Name | Institut National de la Santé Et de la Recherche Médicale, France |
Overall Officials
Sequence: | 29268557 |
Role | Principal Investigator |
Name | Jean-Pierre BLETON, PhD |
Affiliation | Fondation A. de Rothschild |
Design Group Interventions
Sequence: | 68107531 | Sequence: | 68107532 |
Design Group Id | 55559414 | Design Group Id | 55559413 |
Intervention Id | 52454969 | Intervention Id | 52454969 |
Eligibilities
Sequence: | 30747755 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion criteria for patients with writer's cramp
Patient with writer's cramp and writing speed <140 letters / min Non inclusion criteria for patients with writer's cramp Patients whose writer's cramp has no impact on the handwriting and has kept a writing speed> 140 letters per minute. Inclusion criteria for control subjects •> 18 years old Without writer's cramp Non inclusion criteria for control subjects Tremor of writing Matching criteria between cases and control patients Age (± 5 years) |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254122065 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Actual Duration | 9 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Designs
Sequence: | 30494038 |
Allocation | Non-Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Other |
Time Perspective | |
Masking | None (Open Label) |
Responsible Parties
Sequence: | 28860318 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797625
2017-05-04
https://zephyrnet.com/?p=NCT03797625
NCT03797625https://www.clinicaltrials.gov/study/NCT03797625?tab=tablechang jian hua, PDchangjianhua@163.com18017312689The aim of this study is to explore whether endostar combined with IP as treatment could improve progression-free surial time (PFS) and to evaluate the safety of the chemotherapy regimens
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-09 |
Start Month Year | May 4, 2017 |
Primary Completion Month Year | December 31, 2020 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-09 |
Detailed Descriptions
Sequence: | 20727186 |
Description | This study is to explore whether endostar combined with IP as treatment could improve progression-free surial time (PFS) and to evaluate the safety of the chemotherapy regimens used as second-line treatment of advanced esophageal squamous cell carcinomas |
Facilities
Sequence: | 200159423 |
Status | Recruiting |
Name | Cancer hospital Fudan University |
City | Shanghai |
State | Shanghai |
Zip | 200032 |
Country | China |
Facility Contacts
Sequence: | 28113731 |
Facility Id | 200159423 |
Contact Type | primary |
Name | Chang jian hua, PD |
Browse Interventions
Sequence: | 96074204 | Sequence: | 96074205 | Sequence: | 96074206 | Sequence: | 96074207 | Sequence: | 96074208 | Sequence: | 96074209 | Sequence: | 96074210 | Sequence: | 96074211 | Sequence: | 96074212 | Sequence: | 96074213 | Sequence: | 96074214 | Sequence: | 96074215 | Sequence: | 96074216 |
Mesh Term | Cisplatin | Mesh Term | Irinotecan | Mesh Term | Endostar protein | Mesh Term | Antineoplastic Agents | Mesh Term | Topoisomerase I Inhibitors | Mesh Term | Topoisomerase Inhibitors | Mesh Term | Enzyme Inhibitors | Mesh Term | Molecular Mechanisms of Pharmacological Action | Mesh Term | Angiogenesis Inhibitors | Mesh Term | Angiogenesis Modulating Agents | Mesh Term | Growth Substances | Mesh Term | Physiological Effects of Drugs | Mesh Term | Growth Inhibitors |
Downcase Mesh Term | cisplatin | Downcase Mesh Term | irinotecan | Downcase Mesh Term | endostar protein | Downcase Mesh Term | antineoplastic agents | Downcase Mesh Term | topoisomerase i inhibitors | Downcase Mesh Term | topoisomerase inhibitors | Downcase Mesh Term | enzyme inhibitors | Downcase Mesh Term | molecular mechanisms of pharmacological action | Downcase Mesh Term | angiogenesis inhibitors | Downcase Mesh Term | angiogenesis modulating agents | Downcase Mesh Term | growth substances | Downcase Mesh Term | physiological effects of drugs | Downcase Mesh Term | growth inhibitors |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Conditions
Sequence: | 52185503 |
Name | Esophageal Squamous Cell Carcinoma |
Downcase Name | esophageal squamous cell carcinoma |
Id Information
Sequence: | 40169083 |
Id Source | org_study_id |
Id Value | ENDO-SH-002 |
Countries
Sequence: | 42580674 |
Name | China |
Removed | False |
Design Groups
Sequence: | 55609137 |
Group Type | Experimental |
Title | Endostar Combined With IP |
Description | Endostar15mg/m2 Irinotecan 60mg/m2,D1,8 DDP 60mg/m2,D1 |
Interventions
Sequence: | 52499445 | Sequence: | 52499446 | Sequence: | 52499447 |
Intervention Type | Drug | Intervention Type | Drug | Intervention Type | Drug |
Name | Irinotecan | Name | DDP | Name | Endostar |
Description | 60mg/m2,D1,8 | Description | 60mg/m2,D1 | Description | 15mg/d,d1-d7 civ |
Design Outcomes
Sequence: | 177432083 |
Outcome Type | primary |
Measure | Progression Free Survival |
Time Frame | from the first cycle of treatment (day one) to two month after the last cycle |
Browse Conditions
Sequence: | 193540191 | Sequence: | 193540192 | Sequence: | 193540193 | Sequence: | 193540194 | Sequence: | 193540195 | Sequence: | 193540196 | Sequence: | 193540197 | Sequence: | 193540198 | Sequence: | 193540199 | Sequence: | 193540200 | Sequence: | 193540201 | Sequence: | 193540202 | Sequence: | 193540203 | Sequence: | 193540204 | Sequence: | 193540205 |
Mesh Term | Carcinoma | Mesh Term | Carcinoma, Squamous Cell | Mesh Term | Esophageal Squamous Cell Carcinoma | Mesh Term | Neoplasms, Glandular and Epithelial | Mesh Term | Neoplasms by Histologic Type | Mesh Term | Neoplasms | Mesh Term | Neoplasms, Squamous Cell | Mesh Term | Esophageal Neoplasms | Mesh Term | Gastrointestinal Neoplasms | Mesh Term | Digestive System Neoplasms | Mesh Term | Neoplasms by Site | Mesh Term | Head and Neck Neoplasms | Mesh Term | Digestive System Diseases | Mesh Term | Esophageal Diseases | Mesh Term | Gastrointestinal Diseases |
Downcase Mesh Term | carcinoma | Downcase Mesh Term | carcinoma, squamous cell | Downcase Mesh Term | esophageal squamous cell carcinoma | Downcase Mesh Term | neoplasms, glandular and epithelial | Downcase Mesh Term | neoplasms by histologic type | Downcase Mesh Term | neoplasms | Downcase Mesh Term | neoplasms, squamous cell | Downcase Mesh Term | esophageal neoplasms | Downcase Mesh Term | gastrointestinal neoplasms | Downcase Mesh Term | digestive system neoplasms | Downcase Mesh Term | neoplasms by site | Downcase Mesh Term | head and neck neoplasms | Downcase Mesh Term | digestive system diseases | Downcase Mesh Term | esophageal diseases | Downcase Mesh Term | gastrointestinal diseases |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48332349 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Fudan University |
Overall Officials
Sequence: | 29292998 | Sequence: | 29292999 |
Role | Principal Investigator | Role | Principal Investigator |
Name | chang jian hua, PD | Name | wang hui jie, doctor |
Affiliation | PI | Affiliation | SUBI |
Central Contacts
Sequence: | 12012305 |
Contact Type | primary |
Name | chang jian hua, PD |
Phone | 18017312689 |
changjianhua@163.com | |
Role | Contact |
Design Group Interventions
Sequence: | 68168198 | Sequence: | 68168199 | Sequence: | 68168200 |
Design Group Id | 55609137 | Design Group Id | 55609137 | Design Group Id | 55609137 |
Intervention Id | 52499445 | Intervention Id | 52499446 | Intervention Id | 52499447 |
Eligibilities
Sequence: | 30773587 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 75 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Histologically proven primary thoracic esophageal squamous cell carcinoma According to the esophageal AJCC2009 7th to determine new stage IV esophageal cancer The subject has PD after first-line chemotherapy or radiation within a year Presence of at least one index lesion measurable by CT scan or MRI according to RECIST 1.1 Can eat more than liquid diet; No signs before esophageal perforation 18~75 years PS:0-1 Life expectancy of ≥ 3 months ANC ≥ 2×109/L,PLT ≥ 100×109/L,Hb ≥ 90g/L TB ≤ UNL; ALT/AST ≤ 2.5×UNL,AKP ≤ 5×UNL Ccr≤ UNL,Scr≥60 mL/min Normal electrocardiogram (ecg), the body had no unheal wounds Radiotherapy before within the scope of the normal dose and not affect subsequent treatment Prior to biological agents, especially e. coli genetically engineered products without severe allergic reactions Signed written informed consent Exclusion Criteria: Breast-feeding or pregnant women, no effective contraception if risk of conception exists Chronic diarrhea, enteritis, intestine obstruction which are not under control Esophageal obstruction cannot eat liquid completely, esophagus have deep ulcer perforation or hematemesis; Esophageal cancer common complications such as anastomotic leakage, serious lung complications, etc. A second primary tumor (except skin basal cell carcinoma) The original serious heart disease, including: higher risk of congestive heart failure, unable to control arrhythmia, unstable angina, myocardial infarction, severe valvular heart disease, and resistant hypertension With uncontrol nerve, mental illness or mental disorders, compliance is poor, can't cooperate with accounts and response to treatment; Primary brain tumors or CNS metastases illness did not get a control, has obvious cranial hypertension or nerve mental symptoms With bleeding tendency Has inherited bleeding evidence of physical or blood coagulation disorder With clear chemotherapy drug allergy Other researchers believe that patients should not participate in this testing – |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253952757 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 75 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Designs
Sequence: | 30519718 |
Allocation | Non-Randomized |
Intervention Model | Single Group Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | None (Open Label) |
Intervention Other Names
Sequence: | 26680429 | Sequence: | 26680430 |
Intervention Id | 52499446 | Intervention Id | 52499447 |
Name | Cisplatin | Name | ENDO |
Responsible Parties
Sequence: | 28886019 |
Responsible Party Type | Principal Investigator |
Name | Chang Jian Hua |
Title | Chief Physician |
Affiliation | Fudan University |
Study References
Sequence: | 52078927 |
Pmid | 35380726 |
Reference Type | derived |
Citation | Hu Z, Sun S, Zhao X, Yu H, Wu X, Wang J, Chang J, Wang H. Rh-Endostatin Plus Irinotecan/Cisplatin as Second-Line Therapy for Advanced Esophageal Squamous Cell Carcinoma: An Open-Label, Phase II Study. Oncologist. 2022 Apr 5;27(4):253-e312. doi: 10.1093/oncolo/oyab078. |
]]>
https://zephyrnet.com/NCT03797612
2021-01-31
https://zephyrnet.com/?p=NCT03797612
NCT03797612https://www.clinicaltrials.gov/study/NCT03797612?tab=tableNANANAThis is a multi-center, Phase 2, randomized, double-blind, placebo-controlled study to evaluate the safety and efficacy of brivoligide injection administered intrathecally before surgery in patients with a Pain Catastrophizing Scale (PCS) score ≥16 undergoing primary unilateral total knee arthroplasty.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-06 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2020-07-13 |
Start Month Year | January 2021 |
Primary Completion Month Year | January 2022 |
Verification Month Year | July 2020 |
Verification Date | 2020-07-31 |
Last Update Posted Date | 2020-07-13 |
Detailed Descriptions
Sequence: | 20716302 |
Description | The objective of this study is to evaluate the safety and postoperative pain reducing efficacy of a single preoperative intrathecal administration of brivoligide injection in patients with a Pain Catastrophizing Scale (PCS) score ≥16 undergoing unilateral total knee arthroplasty.
Potential subjects will be prescreened for PCS scores of 16 or greater in advance; pre-qualified patients will be invited to the investigative site for informed consent and full screening within 30 days of randomization. Patients providing informed consent and meeting all study eligibility criteria will be enrolled in the study on the day of surgery (Day 1). Safety assessments will be performed through Day 28; efficacy assessments will be conducted at the follow-up visits and daily via electronic diary by subjects through Day 42. Follow up visits will occur on Days 7, 14, 21, 28, and 42. |
Facilities
Sequence: | 200053310 | Sequence: | 200053311 |
Name | Research Site | Name | Research Site |
City | Sheffield | City | Phoenix |
State | Alabama | State | Arizona |
Zip | 35660 | Zip | 85023 |
Country | United States | Country | United States |
Conditions
Sequence: | 52156519 |
Name | Pain, Postoperative |
Downcase Name | pain, postoperative |
Id Information
Sequence: | 40148226 |
Id Source | org_study_id |
Id Value | ADYX-005 |
Countries
Sequence: | 42557744 |
Name | United States |
Removed | False |
Design Groups
Sequence: | 55577923 | Sequence: | 55577924 |
Group Type | Experimental | Group Type | Placebo Comparator |
Title | Brivoligide Injection 660 mg/6 mL | Title | Placebo 6 mL |
Description | Subjects randomized to the active treatment group will receive a single 660 mg/6 mL intrathecal administration of brivoligide injection as a slow bolus injection just prior to administration of spinal anesthesia, via the same needle. | Description | Subjects randomized to the placebo group will receive a single 6 mL intrathecal injection of placebo as a slow bolus injection just prior to administration of spinal anesthesia, via the same needle. |
Interventions
Sequence: | 52472024 | Sequence: | 52472025 |
Intervention Type | Drug | Intervention Type | Drug |
Name | Brivoligide Injection 660 mg/6 mL | Name | Placebo 6 mL |
Description | Single preoperative intrathecal injection | Description | Single preoperative intrathecal injection |
Keywords
Sequence: | 79848130 | Sequence: | 79848131 | Sequence: | 79848132 |
Name | Knee replacement | Name | TKA | Name | Total Knee Arthroplasty |
Downcase Name | knee replacement | Downcase Name | tka | Downcase Name | total knee arthroplasty |
Design Outcomes
Sequence: | 177328053 | Sequence: | 177328054 | Sequence: | 177328055 | Sequence: | 177328056 | Sequence: | 177328057 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Numerical Rating Scale (NRS) Pain with Walking 15 Meters | Measure | Numerical Rating Scale (NRS) Pain at Rest | Measure | Numerical Rating Scale (NRS) Pain with 90 Degrees Passive Knee Flexion | Measure | Total Postoperative Opioid Use | Measure | Time to Numerical Rating Scale (NRS) Pain ≤ 3 for Worst Pain |
Time Frame | Day 7 to Day 28 | Time Frame | Day 7 to Day 28 | Time Frame | Day 7 to Day 28 | Time Frame | Postoperative through Day 42 | Time Frame | Postoperative through Day 42 |
Description | Least squares mean pain rating (NRS) with walking during the 15-meter walk Day 7 to Day 28 | Description | Least squares mean pain rating (NRS) at rest Day 7 to Day 28 | Description | Least squares mean pain rating (NRS) with passive knee flexion to 90 degrees from Day 7 to Day 28 | Description | Total use of postoperative opioid medications (morphine equivalents) to Day 42 | Description | Time to achieve NRS pain score ≤ 3 for worst pain |
Browse Conditions
Sequence: | 193432134 | Sequence: | 193432135 | Sequence: | 193432136 | Sequence: | 193432137 | Sequence: | 193432138 |
Mesh Term | Pain, Postoperative | Mesh Term | Postoperative Complications | Mesh Term | Pathologic Processes | Mesh Term | Pain | Mesh Term | Neurologic Manifestations |
Downcase Mesh Term | pain, postoperative | Downcase Mesh Term | postoperative complications | Downcase Mesh Term | pathologic processes | Downcase Mesh Term | pain | Downcase Mesh Term | neurologic manifestations |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48306099 |
Agency Class | INDUSTRY |
Lead Or Collaborator | lead |
Name | Adynxx, Inc. |
Design Group Interventions
Sequence: | 68130887 | Sequence: | 68130888 |
Design Group Id | 55577923 | Design Group Id | 55577924 |
Intervention Id | 52472024 | Intervention Id | 52472025 |
Eligibilities
Sequence: | 30757367 |
Gender | All |
Minimum Age | 40 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Score of 16 or greater on the PCS scale Exclusion Criteria: Target knee > 20 degrees valgus or varus deformity, evidence of significant bone loss or ligamentous laxity, or existing major hardware that requires removal during TKA |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254228084 |
Number Of Facilities | 2 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | False |
Minimum Age Num | 40 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 4 |
Designs
Sequence: | 30503592 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Quadruple |
Subject Masked | True |
Caregiver Masked | True |
Investigator Masked | True |
Outcomes Assessor Masked | True |
Intervention Other Names
Sequence: | 26665922 |
Intervention Id | 52472024 |
Name | AYX1 Injection 660 mg/6 mL |
Responsible Parties
Sequence: | 28869870 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797599
2019-03-28
https://zephyrnet.com/?p=NCT03797599
NCT03797599https://www.clinicaltrials.gov/study/NCT03797599?tab=tableNANANAThis study aims to examine whether greater length of mindfulness practice results in more beneficial outcomes.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-12-11 |
Start Month Year | March 28, 2019 |
Primary Completion Month Year | December 5, 2019 |
Verification Month Year | September 2019 |
Verification Date | 2019-09-30 |
Last Update Posted Date | 2019-12-11 |
Detailed Descriptions
Sequence: | 20735944 |
Description | This study will randomise participants to one of three groups: (1) four sessions of medium length mindfulness practice (lasting 20 mins) and 5 mins of an audio book; (2) four sessions of brief mindfulness practice (lasting 5 mins) and 20 mins of an audio book; and (3) a control group who just receive 4 sessions of audio book (lasting 25 mins). In the mindfulness arms, in each session, the participants will receive the audio book prior to the mindfulness practice. Mindfulness levels, and depression, anxiety and stress will be measured by self-report at baseline, session by session, and at post-intervention. |
Facilities
Sequence: | 200245075 |
Name | Canterbury Christ Church University |
City | Tunbridge Wells |
State | Kent |
Zip | TN1 2YG |
Country | United Kingdom |
Conditions
Sequence: | 52208506 | Sequence: | 52208507 |
Name | Mindfulness | Name | Healthy Population |
Downcase Name | mindfulness | Downcase Name | healthy population |
Id Information
Sequence: | 40186444 |
Id Source | org_study_id |
Id Value | S_Strohmaier_29-11-18 |
Countries
Sequence: | 42599939 |
Name | United Kingdom |
Removed | False |
Design Groups
Sequence: | 55635122 | Sequence: | 55635123 | Sequence: | 55635124 |
Group Type | Experimental | Group Type | Active Comparator | Group Type | Placebo Comparator |
Title | 20 minutes of mindfulness practice | Title | 5 minutes of mindfulness practice | Title | Audio book control |
Description | Two sessions a week for two weeks of: 5 minutes listening to audio book excerpts followed by 20 minutes of audio guided mindfulness practice. Participants will be asked not to engage in formal mindfulness practice outside of these sessions during the study. | Description | Two sessions a week for two weeks of: 20 minutes listening to audio book excerpts followed by 5 minutes of audio guided mindfulness practice. Participants will be asked not to engage in formal mindfulness practice outside of these sessions during the study. | Description | Two sessions a week for two weeks of: 25 minutes listening to audio book excerpts (with non mindfulness practice). Participants will be asked not to engage in formal mindfulness practice during the study. |
Interventions
Sequence: | 52522466 | Sequence: | 52522467 | Sequence: | 52522468 | Sequence: | 52522469 | Sequence: | 52522470 |
Intervention Type | Behavioral | Intervention Type | Behavioral | Intervention Type | Other | Intervention Type | Other | Intervention Type | Other |
Name | 20 minutes of mindfulness practice | Name | 5 minutes of mindfulness practice | Name | 5 minute audio book | Name | 20 minute audio book | Name | 25 minute audio book |
Description | A 20 minute audio guided mindfulness of breathing practice per session, for four sessions. | Description | A 5 minute audio guided mindfulness of breathing practice per session, for four sessions. | Description | 5 minutes from an audio book by Bill Bryson ('A Short History of Nearly Everything') per session, for four sessions. | Description | 20 minutes from an audio book by Bill Bryson ('A Short History of Nearly Everything'), per session, for four sessions. | Description | 25 minutes from an audio book by Bill Bryson ('A Short History of Nearly Everything'), per session, for four sessions. |
Design Outcomes
Sequence: | 177512779 | Sequence: | 177512780 | Sequence: | 177512781 | Sequence: | 177512786 | Sequence: | 177512782 | Sequence: | 177512783 | Sequence: | 177512784 | Sequence: | 177512785 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other |
Measure | Change from baseline at post-intervention (week 3) on the Five Factor Mindfulness Questionnaire -15 item version (FFMQ-15) | Measure | Change from baseline at post-intervention (week 3) on the Depression, Anxiety and Stress Scale – 21 item version (DASS-21). | Measure | Sessional Five Factor Mindfulness Questionnaire -15 item version (FFMQ-15) scores. | Measure | Session 4 Toronto Mindfulness Scale (TMS). | Measure | Sessional Depression, Anxiety and Stress Scale – 21 item version (DASS-21) scores | Measure | Session 1 Toronto Mindfulness Scale (TMS). | Measure | Session 2 Toronto Mindfulness Scale (TMS). | Measure | Session 3 Toronto Mindfulness Scale (TMS). |
Time Frame | Post-intervention (3 weeks after baseline). | Time Frame | Post-intervention (3 weeks after baseline). | Time Frame | Baseline, session 2 (week 1), session 3 and 4 (week 2), and post-intervention (week 3). | Time Frame | Session 4 (week 2). | Time Frame | Baseline, session 2 (week 1), session 3 and 4 (week 2), and post-intervention (week 3). | Time Frame | Session 1 (week 1). | Time Frame | Session 2 (week 1). | Time Frame | Session 3 (week 2). |
Description | The Five Factor Mindfulness Questionnaire -15 item version is a self-report measure of mindfulness, producing a total score between 15 and 75, with higher scores indicating greater levels of mindfulness. (Note that the observe subscale will be excluded from the calculation of the total score, as recommended in https://doi.org/10.1002/jclp.21865 and http://dx.doi.org/10.1037/pas0000263 producing a total score between 12 and 60). | Description | The Depression, Anxiety and Stress Scale – 21 is a self-report measure of depression, anxiety and stress, producing a total score between 0 and 63, with higher scores indicating greater symptomatology. | Description | The FFMQ-15 (described above) will be administered at the start of the first session (baseline), immediately after sessions 2 (week 1), 3 (week 2) and 4 (week 2), and at post-intervention (week 3), to examine patterns in changes in mindfulness over the course of the study. | Description | As described above. | Description | The DASS-21 (described above) will be administered at the start of the first session (baseline), immediately after sessions 2 (week 1), 3 (week 2) and 4 (week 2), and at post-intervention (week 3), to to examine patterns in changes over the course of the study. | Description | The TMS is a 13-item self-report measure of state mindfulness that produces scores for curiosity and decentering. The curiosity score ranges from 0 to 24, the decentering score from 0 to 28, and the total score from 0 to 52, with higher scores indicating greater curiosity, decentering and overall state mindfulness respectively. | Description | As described above. | Description | As described above. |
Sponsors
Sequence: | 48354119 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Canterbury Christ Church University |
Overall Officials
Sequence: | 29306205 | Sequence: | 29306206 | Sequence: | 29306207 |
Role | Study Director | Role | Study Director | Role | Principal Investigator |
Name | Fergal Jones, PhD, PsychD | Name | James Cane, PhD | Name | Sarah Strohmaier, MSc |
Affiliation | Canterbury Christ Church University | Affiliation | Canterbury Christ Church University | Affiliation | Canterbury Christ Church University |
Design Group Interventions
Sequence: | 68199727 | Sequence: | 68199728 | Sequence: | 68199729 | Sequence: | 68199730 | Sequence: | 68199731 |
Design Group Id | 55635122 | Design Group Id | 55635123 | Design Group Id | 55635122 | Design Group Id | 55635123 | Design Group Id | 55635124 |
Intervention Id | 52522466 | Intervention Id | 52522467 | Intervention Id | 52522468 | Intervention Id | 52522469 | Intervention Id | 52522470 |
Eligibilities
Sequence: | 30787110 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
Members of the general public, especially university students or staff. Exclusion Criteria: Currently experiencing significant difficulties with their mental wellbeing. |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253990033 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Actual Duration | 8 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 1 |
Number Of Other Outcomes To Measure | 6 |
Designs
Sequence: | 30533180 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Basic Science |
Time Perspective | |
Masking | None (Open Label) |
Masking Description | Participants will be masked to the extent that they will not be told which group they have been allocated to nor the exact nature of the the three groups. However, they will be aware of the exercises they are asked to undertake. |
Responsible Parties
Sequence: | 28899473 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797586
2019-05-01
https://zephyrnet.com/?p=NCT03797586
NCT03797586https://www.clinicaltrials.gov/study/NCT03797586?tab=tableNANANAApproximately 70-80% of patients with advanced disease will be affected by moderate to severe pain. Opioid analgesics represented by morphine and oxycodone are the cornerstone of cancer-pain management, and recommended for use in the management of moderate to severe cancer pain according to WHO Cancer Pain Relief Guidelines. One view is that a trial of systemic opioid therapy should be administered to all cancer patients with pain of moderate or greater severity regardless of the pain mechanism. Although opioids analgesics do work well as relieving pain and improving quality of life via their action at opioid receptors in the central nervous system (CNS) and the peripheral nervous system, they also have powerful adverse effects. The overall occurrence of opioid-related adverse drug events has ranged from1.8% to 13.6%. Opioid-induced constipation (OIC), one of the most prevalent adverse events (AEs) in patients receiving opioid analgesics, defined as a change in baseline bowel habits or defecatory patterns following initiation, alteration, or increase in opioid therapy. The prevalence of OIC has been estimated to affect 41% of patients with chronic noncancer pain taking opioids and 94% of cancer patients taking opioids for pain. Unlike many other opioid-related AEs, OIC is persistent and rarely tolerated. OIC impacts pain control, patients’ quality of life and may cause patients to reduce the dose or discontinue opioid use.
Acupuncture, a traditional Chinese medicine, has been used to treat gastrointestinal disease including constipation for thousands of years. Two systematic reviews concluded that acupuncture can improve spontaneous bowel movements for functional constipation, and our recent study indicated that electroacupuncture(EA) could increase complete spontaneous bowel movements and is safe for chronic severe functional constipation. Acupuncture could improve gastrointestinal function via facilitating gastrointestinal motility. Currently, there is little detailed information available regarding the acupuncture use for OIC. The objective of this study is to assess the efficacy and safety of EA for OIC in patients with cancer.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-05 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2022-07-06 |
Start Month Year | May 1, 2019 |
Primary Completion Month Year | October 16, 2021 |
Verification Month Year | July 2022 |
Verification Date | 2022-07-31 |
Last Update Posted Date | 2022-07-06 |
Facilities
Sequence: | 198627730 |
Name | Guang An Men Hospital |
City | Beijing |
Zip | 100053 |
Country | China |
Conditions
Sequence: | 51788697 |
Name | Opioid-induced Constipation in Patients With Cancer |
Downcase Name | opioid-induced constipation in patients with cancer |
Id Information
Sequence: | 39854215 |
Id Source | org_study_id |
Id Value | 2018-164-KY-01 |
Countries
Sequence: | 42253048 |
Name | China |
Removed | False |
Design Groups
Sequence: | 55208912 | Sequence: | 55208913 |
Group Type | Experimental | Group Type | Sham Comparator |
Title | Electroacupuncture group | Title | Sham electroacupuncture group |
Description | Bilateral ST25,SP14, ST37 will be used in the EA group. For ST25 and SP14, 0.30×50mm or 0.30×75mm needles will be vertically inserted to the muscle layer of the abdominal , where patients will feel sharp pain and acupuncturists will feel resistance from the needle tip. For ST37, 0.30×40 mm needles will be vertically inserted approximately 15 mm deep, followed by three-time manipulation of even lifting and twisting method to elicit the sensation of deqi. Then paired alligator clips of the EA apparatus will be attached to the needle holders of the bilateral ST25, SP14, and ST37. EA stimulation will be retained for 30 minutes with a continuous wave of 10 Hz and current intensity of 0.5 to 4 mA. | Description | Bilateral sham ST25, SP14, and ST37 will be used in the SA group. After sterilizing the skin, 0.30×40mm needles will be straightly inserted at the sham points about 2-3mm until they can be fixed on the skin when attached by the alligator clips. No manipulation will be used, and no deqi sensation are elicited for all sham points. The bilateral sham ST25, SP14, and ST37 points will be attached by the same EA apparatus with a continuous wave of 10 Hz and current intensity of 0.1 to 0.2 mA for 30 minutes with only the initial 30 seconds on. |
Interventions
Sequence: | 52111191 | Sequence: | 52111192 |
Intervention Type | Other | Intervention Type | Other |
Name | Electroacupuncture group | Name | Sham electroacupuncture group |
Description | Bilateral Tianshu (ST25), Fujie (SP14), Shangjuxu (ST37) will be used in the EA group. With the local skin of the patients was routinely sterilized in a prone position in relaxation, acupuncturists will insert needles into the acupuncture points. For ST25 and SP14, 0.30×50mm or 0.30×75mm needles will be vertically inserted to the muscle layer of the abdominal wall, where participants will feel sharp pain and acupuncturists will feel resistance from the needle tip. For ST37, 0.30×40 mm needles will be vertically inserted approximately 15 mm deep, followed by three-time manipulation of even lifting and twisting method to elicit the sensation of deqi. Then paired alligator clips of the EA apparatus will be attached to the needle holders of the bilateral ST25, SP14, and ST37. EA stimulation will be retained for 30 minutes with a continuous wave of 10 Hz and current intensity of 0.5 to 4 mA. | Description | Bilateral sham ST25, SP14, and ST37 will be used in the SA group. After sterilizing the skin, 0.30×40mm needles will be straightly inserted at the sham points about 2-3mm until they can be fixed on the skin when attached by the alligator clips. No manipulation will be used, and no deqi sensation are elicited for all sham points. The bilateral sham ST25, SP14, and ST37 points will be attached by the same EA apparatus with a continuous wave of 10 Hz and current intensity of 0.1 to 0.2 mA for 30 minutes with only the initial 30 seconds on. |
Keywords
Sequence: | 79240632 |
Name | electroacupuncture;opioid-induced constipation ,cancer |
Downcase Name | electroacupuncture;opioid-induced constipation ,cancer |
Design Outcomes
Sequence: | 176147714 | Sequence: | 176147715 | Sequence: | 176147716 | Sequence: | 176147717 | Sequence: | 176147718 | Sequence: | 176147719 | Sequence: | 176147720 | Sequence: | 176147721 | Sequence: | 176147722 | Sequence: | 176147723 | Sequence: | 176147724 | Sequence: | 176147725 | Sequence: | 176147726 | Sequence: | 176147727 | Sequence: | 176147728 | Sequence: | 176147729 | Sequence: | 176147730 | Sequence: | 176147731 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other |
Measure | The proportion of responders | Measure | Change in the mean weekly spontaneous bowel movements (SBMs) from the baseline during weeks 1-8 and weeks 13-16. | Measure | The proportion of patients with ≥3 mean weekly spontaneous bowel movements (SBMs) during weeks 1-8 and weeks 13-16 | Measure | The proportion of patients with an increase of ≥1 mean weekly spontaneous bowel movements (SBMs) from the baseline during weeks 1-8 and weeks 13-16 | Measure | A Change in the mean weekly complete spontaneous bowel movements (CSBMs) from the baseline during weeks 1-8 and weeks 13-16. | Measure | The proportion of patients with ≥3 mean weekly spontaneous bowel movements (CSBMs) during weeks 1-8 and weeks 13-16 | Measure | The proportion of patients with an increase of ≥1 mean weekly spontaneous bowel movements (CSBMs) from the baseline during weeks 1-8 and weeks 13-16 | Measure | A change in the mean Bristol Stool Form Scale score for stool consistency of spontaneous bowel movements (SBMs) from the baseline during weeks 1-8 and weeks 13-16 | Measure | A change in the mean score for the straining of spontaneous bowel movements (SBMs) from the baseline during weeks 1-8 and weeks 13-16 | Measure | A change in the total and subscale score of the Patient Assessment of Constipation-Symptom (PAC-SYM) questionnaire from baseline at weeks 8 and 16 | Measure | A change in the total and subscale scores of the Patient Assessment of Constipation-Quality of Life (PAC-QOL) questionnaires from the baseline at weeks 8 and 16 | Measure | Patients' global assessment of treatment efficacy | Measure | The proportion of patients using rescue medicine and the mean frequency of rescue medicine use per week during weeks 1-8 and weeks 9-16 | Measure | Patients'expectation of the acupuncture efficacy | Measure | The patient blinding assessment | Measure | Incidence of adverse events | Measure | The intensity of cancerous pain evaluation | Measure | The proportion of patients discontinuing the opioid, and those with a ≥30% weekly mean increase or decrease in the dose of opioid from baseline during weeks 1-8 and weeks 9-16 |
Time Frame | weeks 1-8 | Time Frame | weeks 1-8, and weeks 13-16 | Time Frame | weeks 1-8, and weeks 13-16 | Time Frame | weeks 1-8, and weeks 13-16 | Time Frame | weeks 1-8, and weeks 13-16 | Time Frame | weeks 1-8, and weeks 13-16 | Time Frame | weeks 1-8, and weeks 13-16 | Time Frame | weeks 1-8, and weeks 13-16 | Time Frame | weeks 1-8, and weeks 13-16 | Time Frame | week 8 and week 16 | Time Frame | week 8 and week 16 | Time Frame | week 8 and week 16 | Time Frame | weeks 1-8, and weeks 9-16 | Time Frame | at baseline | Time Frame | at week 8 | Time Frame | week 1 to week 16 | Time Frame | at baseline, at weeks 2, 4, 6, 8 and 16. | Time Frame | at week 8 and week 16 |
Description | A responder is defined as a patient that has at least three spontaneous bowel movements (SBMs) per week and an increase of at least one SBM a week from the baseline for at least 6 of the 8 weeks of the treatment period. | Description | An SBM was defined as a bowel movement that occurred without any medication or intervention to assist defection within the previous 24 hours. A bowel movement occurring within 24 hours of an optional assisted method for defecation was not considered to be an SBM. | Description | An SBM was defined as a bowel movement that occurred without any medication or intervention to assist defection within the previous 24 hours. A bowel movement occurring within 24 hours of an optional assisted method for defecation was not considered to be an SBM. | Description | An SBM was defined as a bowel movement that occurred without any medication or intervention to assist defection within the previous 24 hours. A bowel movement occurring within 24 hours of an optional assisted method for defecation was not considered to be an SBM. | Description | An SBM was defined as a bowel movement that occurred without any medication or intervention to assist defection within the previous 24 hours. A bowel movement occurring within 24 hours of an optional assisted method for defecation was not considered to be an SBM. A CSBM was defined as an SBM with the feeling of complete evacuation. | Description | An SBM was defined as a bowel movement that occurred without any medication or intervention to assist defection within the previous 24 hours. A bowel movement occurring within 24 hours of an optional assisted method for defecation was not considered to be an SBM. A CSBM was defined as an SBM with the feeling of complete evacuation. | Description | An SBM was defined as a bowel movement that occurred without any medication or intervention to assist defection within the previous 24 hours. A bowel movement occurring within 24 hours of an optional assisted method for defecation was not considered to be an SBM. A CSBM was defined as an SBM with the feeling of complete evacuation. | Description | For stool consistency, each patient was asked to record their stool consistency according to the Bristol Stool Form Scale, on the following seven points scale. (scored from 1 to 7 for stool types 1 to 7, respectively) | Description | For assessment of straining of SBM, each patient was asked to rate his/her score for straining using the following five-point scale: not at all difficulty (0), a little bit difficulty (1), moderately difficulty (2), quite a bit difficulty (3), extremely difficulty (4). | Description | The PAC-SYM is a 12-item evaluative questionnaire for the chronic constipation, which consists of 4-item abdominal, 3-item rectal, and 5-item stool subscales. Each item score ranges from 0 to 4 in the 2 weeks (14 days) prior to assessment. The, where 0 = symptom absent, 1 = mild,2 = moderate,3 = severe and 4 = very severe. Lower scores indicate a lower symptom burden. Each subscale score will be calculated as the mean of the completed items for that subscale. The total score will be calculated as the mean of all completed items. | Description | The PAC-QOL is a 28-item self-reported instrument for assessing the burden of constipation on patients' everyday functioning and well-being in the 2 weeks (14 days) prior to assessment. It is divided into four subscales: physical discomfort (items 1-4), psychosocial discomfort (items 5-12), worries/concerns (items 13-23), and satisfaction (items 24 to 28). Each of the item scores ranges from 0 (not at all) to 4 (extremely), with lower scores indicating a better quality of life. For each visit, individual subscale scores will be calculated as the mean of the completed items for that subscale. | Description | each patient was asked to rate his/her efficacy of treatment using the following 7-point self-reporting scale: markedly worse (1), moderately worse (2),slightly worse (3), no change (4), slightly improved (5), moderately improved (6), markedly improved (7). | Description | The proportion of patients using rescue medicine will be compared between groups during weeks 1-8, and weeks 9-16. The mean frequency of using rescue medicine per week during weeks 1-8 equals the total of rescue medicine consumption divided by 8. The mean frequency of using rescue medicine per week during weeks 9-16 equals the total of rescue medicine consumption divided by 8. | Description | Participants will be asked to answer the following questions before the intervention: "Do you think acupuncture will be effective in treating the disease in general?" "Do you think acupuncture will be effective in improving the OIC?" and "which acupuncture modalities do you prefer, EA or SA?" For each question, patients will choose one of the following answers: "unclear/whatever", "EA", or "SA" | Description | Five minutes after the end of any treatment in the eighth week the patients will be asked to answer the following question: "Is traditional EA the acupuncture modality that you have received?". | Description | All adverse events (AEs) t will be recorded throughout the whole trial in case report form. AEs will be categorized as treatment-related (e.g., broken needle, dizziness, fainting, localized hematoma, localized infection or abscess, or some discomforts after acupuncture) and non-treatment-related. Detailed information regarding AEs and serious adverse events (SAEs)-including the name, onset and end date, intensity, relationship with acupuncture and outcome-will be recorded. | Description | The mean cancerous pain intensity and worst cancerous pain intensity during the preceding week will be evaluated by 11 grades (from "0=no pain" to "10=worst pain (the strongest pain ever experienced)" at baseline, as well as weeks 2, 4, 6, 8 and 16. | Description | The proportion of patients discontinuing the opioid, and those with increase/decrease from baseline of ≥30% opioid usage per week will be compared between groups during weeks 1-8, and weeks 9-16 |
Browse Conditions
Sequence: | 191945859 | Sequence: | 191945860 | Sequence: | 191945861 | Sequence: | 191945862 | Sequence: | 191945863 | Sequence: | 191945864 | Sequence: | 191945865 |
Mesh Term | Constipation | Mesh Term | Opioid-Induced Constipation | Mesh Term | Signs and Symptoms, Digestive | Mesh Term | Narcotic-Related Disorders | Mesh Term | Substance-Related Disorders | Mesh Term | Chemically-Induced Disorders | Mesh Term | Mental Disorders |
Downcase Mesh Term | constipation | Downcase Mesh Term | opioid-induced constipation | Downcase Mesh Term | signs and symptoms, digestive | Downcase Mesh Term | narcotic-related disorders | Downcase Mesh Term | substance-related disorders | Downcase Mesh Term | chemically-induced disorders | Downcase Mesh Term | mental disorders |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 47962730 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Guang'anmen Hospital of China Academy of Chinese Medical Sciences |
Overall Officials
Sequence: | 29059801 |
Role | Study Chair |
Name | Zhishun Liu |
Affiliation | China Academy of Chinese Medicine Sciences |
Design Group Interventions
Sequence: | 67687601 | Sequence: | 67687602 |
Design Group Id | 55208912 | Design Group Id | 55208913 |
Intervention Id | 52111191 | Intervention Id | 52111192 |
Eligibilities
Sequence: | 30540862 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 85 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Cancer patients who conformed to all the following conditions will be further screened for eligibility: Cancer patients must meet the Rome IV[1] diagnostic criteria for OIC: New or worsening symptoms of constipation following initiation, alteration, or increase in opioid treatment. For patients with a history of chronic functional constipation, he/she must have worsening symptoms of constipation when the opioid therapy is initiated, changed, or the dose is increased; Exclusion Criteria: Participants who fulfill any of the following criteria will be excluded: Patients diagnosed with clinically significant abnormal defecation due to structural abnormalities of the gastrointestinal tract and other tissues related to gastrointestinal tract (not including OIC): inflammatory bowel disease, rectal prolapse, gastrointestinal obstruction, peritoneal metastasis, or peritoneal tumor at the time of enrollment; |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254203782 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Actual Duration | 29 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 85 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 12 |
Number Of Other Outcomes To Measure | 5 |
Designs
Sequence: | 30289396 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Double |
Subject Masked | True |
Outcomes Assessor Masked | True |
Pending Results
Sequence: | 1487044 | Sequence: | 1487045 |
Event | Release | Event | Reset |
Event Date Description | August 7, 2022 | Event Date Description | July 7, 2023 |
Event Date | 2022-08-07 | Event Date | 2023-07-07 |
Responsible Parties
Sequence: | 28668356 |
Responsible Party Type | Principal Investigator |
Name | Liu Zhishun |
Title | Principal Investigator |
Affiliation | Guang'anmen Hospital of China Academy of Chinese Medical Sciences |
Study References
Sequence: | 51684083 |
Pmid | 35492306 |
Reference Type | derived |
Citation | Wang W, Wang X, Liu Y, Sun Y, Liu X, Yan Y, Liu Z. Effects of Electroacupuncture on Opioid-Induced Constipation in Patients With Cancer: Study Protocol for a Multicenter Randomized Controlled Trial. Front Med (Lausanne). 2022 Apr 13;9:818258. doi: 10.3389/fmed.2022.818258. eCollection 2022. |
]]>
https://zephyrnet.com/NCT03797573
2014-01-20
https://zephyrnet.com/?p=NCT03797573
NCT03797573https://www.clinicaltrials.gov/study/NCT03797573?tab=tableNANANAPrevious studies showed that transcranial direct current stimulation (tDCS) transiently improves performance of motor function in stroke patients, as well as decrease muscle hypertonia. In severely brain injured patients with disorders of consciousness (DOC), a single stimulation over the left dorsolateral prefrontal cortex has shown to improve patients’ sign of consciousness. Nevertheless, other brain areas could be stimulated in order to manage other symptoms occurring in this population of patients, such as muscle hypertonia. In this study, investigators will assess the effects of bilateral fronto-central tDCS on spasticity as measured with the Modified Ashworth Scale (MAS) and on the Coma Recovery Scale-Revised (CRS-R) scores in patients with DOC in a double-blind sham-controlled experimental design.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-03 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-09 |
Start Month Year | January 20, 2014 |
Primary Completion Month Year | June 28, 2014 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-09 |
Detailed Descriptions
Sequence: | 20741271 |
Description | Following severe brain damage and coma, some patients may remain in a vegetative state (VS) or minimally conscious state (MCS). At present, there are no evidence-based guidelines regarding the treatment of patients with disorders of consciousness (DOC). A previous study showed that a single stimulation (using transcranial direct current stimulation – tDCS) of the left prefrontal cortex induces an behavioral improvement in some patients in DOC. Nevertheless, patients with DOC suffer from other invalidating dysfunctions such as spasticity (muscle hypertonia). In sroke patients, the inhibition of the motor cortex through cathodes placed over the motor region showed to reduce spasticity.
In this study, investigators aim to assess the effect of single session of transcranial direct current stimulation (tDCS) over right and left fronto-central areas (using 2 anodes and 2 cathodes), on the level of hypertonia and the level of consciousness of patients with DOC, in a double blind randomized sham controlled study. The anodes will be placed over F3 and F4, and the cathodes over C3 and C4. tDCS is a form of safe non-invasive cortical stimulation, modulating cortical excitability under the electrodes, via weak polarizing currents. It has been reported that anodal tDCS transiently improves motor functions in healthy subjects and patients with stroke or Parkinson's disease. By reducing the activity of the motor cortex (cathodes) and increasing the activity of the prefrontal cortex (anodes) we expect to observe a better motor function in patients with DOC. |
Facilities
Sequence: | 200280885 |
Name | University of Liege |
City | Liege |
Zip | 4000 |
Country | Belgium |
Conditions
Sequence: | 52221788 | Sequence: | 52221789 | Sequence: | 52221790 | Sequence: | 52221791 |
Name | Vegetative State | Name | Minimally Conscious State | Name | Spasticity, Muscle | Name | Disorder of Consciousness |
Downcase Name | vegetative state | Downcase Name | minimally conscious state | Downcase Name | spasticity, muscle | Downcase Name | disorder of consciousness |
Id Information
Sequence: | 40195808 |
Id Source | org_study_id |
Id Value | 2014/280B |
Countries
Sequence: | 42609787 |
Name | Belgium |
Removed | False |
Design Groups
Sequence: | 55650078 | Sequence: | 55650077 |
Group Type | Sham Comparator | Group Type | Active Comparator |
Title | sham tDCS | Title | active tDCS |
Description | Patients will receive sham tDCS (5 seconds of stimulation) during 20 minutes preceded and followed by a clinical assessment (Modified Ashworth Scale and Coma Recovery Scale-Revised) and neurophysiological assessment (8 channels EEG). | Description | Patients will receive tDCS (bilateral fronto-central stimulation) during 20 minutes preceded and followed by a clinical assessment (Modified Ashworth Scale and Coma Recovery Scale-Revised) and neurophysiological assessment (8 channels EEG). |
Interventions
Sequence: | 52535586 | Sequence: | 52535587 |
Intervention Type | Device | Intervention Type | Device |
Name | tDCS | Name | sham tDCS |
Description | tDCS will be applied during 20 minutes with a current of 1 mA preceded and followed by a behavioral assessments (Modified Ashworth Scale and Coma Recovery Scale Revised) and an EEG. The anodes will be placed over F3 and F4 and the cathodes over C3 and C4. | Description | Indentical to the active tDCS, except that the stimulation is terminated after 5 seconds. |
Keywords
Sequence: | 79942110 | Sequence: | 79942111 | Sequence: | 79942112 | Sequence: | 79942113 | Sequence: | 79942114 | Sequence: | 79942115 |
Name | transcranial direct current stimulation | Name | disorder of consciousness | Name | muscle hypertonia | Name | spasticity | Name | vegetative state | Name | minimally conscious state |
Downcase Name | transcranial direct current stimulation | Downcase Name | disorder of consciousness | Downcase Name | muscle hypertonia | Downcase Name | spasticity | Downcase Name | vegetative state | Downcase Name | minimally conscious state |
Design Outcomes
Sequence: | 177562303 | Sequence: | 177562304 | Sequence: | 177562305 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Change in MAS scores | Measure | Change in the CRS-R total score | Measure | Change in brain oscillations |
Time Frame | baseline and directly after tDCS (20 minutes) | Time Frame | Baseline and directly after the tDCS (20 minutes)] | Time Frame | Baseline and directly after the tDCS (20 minutes) |
Description | Modified Ashworth Scale (MAS) will by assessed before and after tDCS (active and sham). Comparison of treatment effect (MAS score after tDCS minus before) between active and sham tDCS. The MAS is a 5 points scale going from 0 (no spasticity) and 5 (extreme spasticity). | Description | Coma Recovery Scale Revised (CRS-R) will be performed before and after tDCS (anodal and sham). Comparison of the treatment effect (CRS-R total score score after tDCS minus before) between real and sham tDCS. The CRS-R is 23 points scale with 6 sub-scales (lower scores refer to reflexes, while higher scores refer to more complex behaviors). The total score is the sum of the scores in the 6 sub-scales. | Description | 8 channels electroencephalography (EEG) will be record before and after tDCS to record potential cortical changes induce by the stimulation. EEG power will be compared in different bandwidths (delta, theta, alpha, beta). |
Browse Conditions
Sequence: | 193679441 | Sequence: | 193679442 | Sequence: | 193679443 | Sequence: | 193679444 | Sequence: | 193679445 | Sequence: | 193679446 | Sequence: | 193679447 | Sequence: | 193679448 | Sequence: | 193679449 | Sequence: | 193679450 | Sequence: | 193679451 | Sequence: | 193679452 | Sequence: | 193679453 | Sequence: | 193679454 | Sequence: | 193679455 | Sequence: | 193679456 |
Mesh Term | Muscle Spasticity | Mesh Term | Consciousness Disorders | Mesh Term | Persistent Vegetative State | Mesh Term | Muscle Hypertonia | Mesh Term | Muscular Diseases | Mesh Term | Musculoskeletal Diseases | Mesh Term | Neuromuscular Manifestations | Mesh Term | Neurologic Manifestations | Mesh Term | Nervous System Diseases | Mesh Term | Neurobehavioral Manifestations | Mesh Term | Neurocognitive Disorders | Mesh Term | Mental Disorders | Mesh Term | Brain Damage, Chronic | Mesh Term | Brain Diseases | Mesh Term | Central Nervous System Diseases | Mesh Term | Unconsciousness |
Downcase Mesh Term | muscle spasticity | Downcase Mesh Term | consciousness disorders | Downcase Mesh Term | persistent vegetative state | Downcase Mesh Term | muscle hypertonia | Downcase Mesh Term | muscular diseases | Downcase Mesh Term | musculoskeletal diseases | Downcase Mesh Term | neuromuscular manifestations | Downcase Mesh Term | neurologic manifestations | Downcase Mesh Term | nervous system diseases | Downcase Mesh Term | neurobehavioral manifestations | Downcase Mesh Term | neurocognitive disorders | Downcase Mesh Term | mental disorders | Downcase Mesh Term | brain damage, chronic | Downcase Mesh Term | brain diseases | Downcase Mesh Term | central nervous system diseases | Downcase Mesh Term | unconsciousness |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48366651 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | University of Liege |
Design Group Interventions
Sequence: | 68217722 | Sequence: | 68217723 |
Design Group Id | 55650077 | Design Group Id | 55650078 |
Intervention Id | 52535586 | Intervention Id | 52535587 |
Eligibilities
Sequence: | 30794857 |
Gender | All |
Minimum Age | 16 Years |
Maximum Age | 75 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
post comatose patients Exclusion Criteria: premorbid neurology antecedent |
Adult | True |
Child | True |
Older Adult | True |
Calculated Values
Sequence: | 254004540 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Actual Duration | 5 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 16 |
Maximum Age Num | 75 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 2 |
Designs
Sequence: | 30540897 |
Allocation | Randomized |
Intervention Model | Crossover Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Quadruple |
Subject Masked | True |
Caregiver Masked | True |
Investigator Masked | True |
Outcomes Assessor Masked | True |
Responsible Parties
Sequence: | 28907217 |
Responsible Party Type | Principal Investigator |
Name | Aurore Thibaut |
Title | Principal Investigator |
Affiliation | University of Liege |
Study References
Sequence: | 52118558 |
Pmid | 24574549 |
Reference Type | background |
Citation | Thibaut A, Bruno MA, Ledoux D, Demertzi A, Laureys S. tDCS in patients with disorders of consciousness: sham-controlled randomized double-blind study. Neurology. 2014 Apr 1;82(13):1112-8. doi: 10.1212/WNL.0000000000000260. Epub 2014 Feb 26. |
]]>
https://zephyrnet.com/NCT03797560
2019-03-22
https://zephyrnet.com/?p=NCT03797560
NCT03797560https://www.clinicaltrials.gov/study/NCT03797560?tab=tableNANANAFibromyalgia is a chronic debilitating musculoskeletal pain syndrome. Pregabalin is the only medication that has been approved to treat fibromyalgia in China. Currently, there has been a growing interest in the development of non-pharmacological therapies. Ba-Duan-Jin is an ancient Chinese exercise for health promotion yet easy to learn. Findings from our previous study showed an effectiveness and good safety of Ba-Duan-Jin in patients with fibromyalgia. This study is to evaluate the effectiveness comparison of Ba-Duan-Jin and pregabalin in managing fibromyalgia symptoms experienced by Chinese patients.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-06 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2022-12-06 |
Start Month Year | March 22, 2019 |
Primary Completion Month Year | October 31, 2021 |
Verification Month Year | December 2022 |
Verification Date | 2022-12-31 |
Last Update Posted Date | 2022-12-06 |
Facilities
Sequence: | 198883323 |
Name | Jiao Juan |
City | Beijing |
State | Beijing |
Zip | 100053 |
Country | China |
Browse Interventions
Sequence: | 95442541 | Sequence: | 95442554 | Sequence: | 95442549 | Sequence: | 95442542 | Sequence: | 95442543 | Sequence: | 95442544 | Sequence: | 95442545 | Sequence: | 95442546 | Sequence: | 95442547 | Sequence: | 95442548 | Sequence: | 95442550 | Sequence: | 95442551 | Sequence: | 95442552 | Sequence: | 95442553 |
Mesh Term | Pregabalin | Mesh Term | Psychotropic Drugs | Mesh Term | Molecular Mechanisms of Pharmacological Action | Mesh Term | Analgesics | Mesh Term | Sensory System Agents | Mesh Term | Peripheral Nervous System Agents | Mesh Term | Physiological Effects of Drugs | Mesh Term | Anticonvulsants | Mesh Term | Calcium Channel Blockers | Mesh Term | Membrane Transport Modulators | Mesh Term | Calcium-Regulating Hormones and Agents | Mesh Term | Anti-Anxiety Agents | Mesh Term | Tranquilizing Agents | Mesh Term | Central Nervous System Depressants |
Downcase Mesh Term | pregabalin | Downcase Mesh Term | psychotropic drugs | Downcase Mesh Term | molecular mechanisms of pharmacological action | Downcase Mesh Term | analgesics | Downcase Mesh Term | sensory system agents | Downcase Mesh Term | peripheral nervous system agents | Downcase Mesh Term | physiological effects of drugs | Downcase Mesh Term | anticonvulsants | Downcase Mesh Term | calcium channel blockers | Downcase Mesh Term | membrane transport modulators | Downcase Mesh Term | calcium-regulating hormones and agents | Downcase Mesh Term | anti-anxiety agents | Downcase Mesh Term | tranquilizing agents | Downcase Mesh Term | central nervous system depressants |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Conditions
Sequence: | 51867114 |
Name | Fibromyalgia |
Downcase Name | fibromyalgia |
Id Information
Sequence: | 39915355 |
Id Source | org_study_id |
Id Value | Z181100001718153 |
Countries
Sequence: | 42312531 |
Name | China |
Removed | False |
Design Groups
Sequence: | 55293089 | Sequence: | 55293090 |
Group Type | Experimental | Group Type | Active Comparator |
Title | Ba-Duan-Jin group | Title | Pregabalin group |
Description | Ba-Duan-Jin therapy: The participants will be guided by a research staff to do the Ba-Duan-Jin therapy for 50 minutes twice weekly for 12 weeks, in the outpatient section of the hospital.
Placebo pregabalin capsules: Pregabalin placebo treatment will be administered at bedtime once a day, starting at 150 mg for the first week, and increase to the dose of 300 mg from the second week. After one week, if 300 mg dose is tolerable, then maintain it for 10 additional weeks, if not, then go back to the 150 mg dose for 10 additional weeks. |
Description | Wellness education and muscle relaxation exercise program: This program will be held for 50 minutes twice weekly for twelve weeks, containing 10-minute wellness education, 10-minute doctor-patient discussion, and 30-minute guided muscle relaxation exercise.
Active pregabalin capsules: As same usage as the placebo pregabalin capsules. |
Interventions
Sequence: | 52186428 | Sequence: | 52186429 |
Intervention Type | Other | Intervention Type | Drug |
Name | Ba-Duan-Jin | Name | Pregabalin capsule |
Description | Ba-Duan-Jin is a common form of "self-health-care" Qigong exercise that has been practiced by Chinese people for at least eight hundred years. It consists of eight sets of simple movements. By combining meditation with slow, graceful movements, deep breathing, and relaxation, Ba-Duan-Jin practitioners believe it has the ability to move vital energy (Qi) throughout the body. Ba-Duan-Jin is also considered to be a multicomponent intervention that integrates physical, psychosocial, emotional, spiritual, and behavioral elements. While the biological mechanisms remain unclear, previous clinical trials have demonstrated that Ba-Duan-Jin can improve sleep quality, physical health, and mental health in patients with various chronic diseases | Description | Pregabalin is one of the three medications (pregabalin, duloxetine, and milnacipran) that have been approved by the Food and Drug Administration (FDA) to treat fibromyalgia in US, and the only medicine that has been approved in China. |
Keywords
Sequence: | 79373829 |
Name | Eight Brocades; Ba-Duan-Jin; Baduanjin; Qigong; Pain |
Downcase Name | eight brocades; ba-duan-jin; baduanjin; qigong; pain |
Design Outcomes
Sequence: | 176386028 | Sequence: | 176386029 | Sequence: | 176386030 | Sequence: | 176386031 | Sequence: | 176386032 | Sequence: | 176386033 | Sequence: | 176386034 | Sequence: | 176386035 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | The change of the Visual Analogue Scale (VAS) for pain from baseline. | Measure | The change of the revised Fibromyalgia Impact Questionnaire (FIQR) from baseline. | Measure | The change of the Multidimensional Fatigue Inventory-20 (MFI-20) from baseline. | Measure | The change of the Pittsburgh Sleep Quality Index (PSQI) from baseline. | Measure | The Beck II Depression Inventory (BDI) | Measure | The change of the Perceived Stress Scale (PSS) from baseline. | Measure | Global Impression of Change (PGIC) questionnaire evaluated at week 12. | Measure | The change of the Short Form-36 Health Status Questionnaire (SF-36) from baseline. |
Time Frame | up to 1 week | Time Frame | Baseline, week 4, week 8, and week 12. | Time Frame | Baseline, week 4, week 8, and week 12. | Time Frame | Baseline, week 4, week 8, and week 12. | Time Frame | Baseline, week 4, week 8, and week 12. | Time Frame | Baseline, week 4, week 8, and week 12. | Time Frame | Week 12. | Time Frame | Baseline, week 4, week 8, and week 12. |
Description | Pain VAS, range, 0 to 100 mm, where higher scores indicated the perceived pain to be more severe. | Description | A self-administered questionnaire with 10 subscales, measuring fibromyalgia symptoms and function domains. FIQR total score ranges from 0 to 100, with higher scores indicating more severe symptoms. | Description | The Multidimensional Fatigue Inventory-20 (MFI-20) measures fatigue severity. The MFI-20 total score ranges from 0 to 80, with higher scores indicate more severe fatigue. | Description | Scores on the Pittsburgh Sleep Quality Index (PSQI) range from 0 to 21, with higher scores indicating worse sleep quality. | Description | The Beck II Depression Inventory (BDI) assesses the severity of depressive symptoms. Scores range from 0 to 39, with higher scores indicate a greater degree of depression severity. | Description | The Perceived Stress Scale (PSS) is for measuring the perception of stress and current levels of experienced stress. Scores range from 0 to 56, with higher total score indicating a greater degree of symptom severity. | Description | A questionnaire determine any change in overall symptom status from the beginning of the study to its conclusion (score range, 1 [very much improved] to 7 [very much worse). | Description | The Short Form-36 Health Status Questionnaire (SF-36), which measured health-related quality of life (range, 0 to 100, with higher scores indicating better perceived health status). |
Browse Conditions
Sequence: | 192254867 | Sequence: | 192254868 | Sequence: | 192254869 | Sequence: | 192254870 | Sequence: | 192254871 | Sequence: | 192254872 | Sequence: | 192254873 |
Mesh Term | Fibromyalgia | Mesh Term | Myofascial Pain Syndromes | Mesh Term | Muscular Diseases | Mesh Term | Musculoskeletal Diseases | Mesh Term | Rheumatic Diseases | Mesh Term | Neuromuscular Diseases | Mesh Term | Nervous System Diseases |
Downcase Mesh Term | fibromyalgia | Downcase Mesh Term | myofascial pain syndromes | Downcase Mesh Term | muscular diseases | Downcase Mesh Term | musculoskeletal diseases | Downcase Mesh Term | rheumatic diseases | Downcase Mesh Term | neuromuscular diseases | Downcase Mesh Term | nervous system diseases |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48036671 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Guang'anmen Hospital of China Academy of Chinese Medical Sciences |
Design Group Interventions
Sequence: | 67784041 | Sequence: | 67784042 |
Design Group Id | 55293089 | Design Group Id | 55293090 |
Intervention Id | 52186428 | Intervention Id | 52186429 |
Eligibilities
Sequence: | 30586823 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 70 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
meet the 1990 American College of Rheumatology (ACR) Research Classification Criteria for fibromyalgia; Exclusion Criteria: had practiced Ba-Duan-Jin, Tai Chi, yoga or other forms of Qigong exercise within 12 months of their recruitment to the study; |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253866118 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Actual Duration | 31 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 70 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 7 |
Designs
Sequence: | 30334847 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Single |
Outcomes Assessor Masked | True |
Intervention Other Names
Sequence: | 26532048 |
Intervention Id | 52186428 |
Name | Baduanjin; Eight Brocades; Eight-Section Brocade |
Responsible Parties
Sequence: | 28713254 |
Responsible Party Type | Principal Investigator |
Name | Juan Jiao |
Title | Deputy chief physician |
Affiliation | Guang'anmen Hospital of China Academy of Chinese Medical Sciences |
Study References
Sequence: | 51759696 |
Pmid | 34292537 |
Reference Type | derived |
Citation | Yang Y, Li YT, Sun YR, Wang J, Li Y, Zhang JH, Jiao J, Jiang Q. Therapeutic Effects of Ba-Duan-Jin versus Pregabalin for Fibromyalgia Treatment: Protocol for a Randomized Controlled Trial. Rheumatol Ther. 2021 Sep;8(3):1451-1462. doi: 10.1007/s40744-021-00341-9. Epub 2021 Jul 22. |
]]>
https://zephyrnet.com/NCT03797547
2018-06-22
https://zephyrnet.com/?p=NCT03797547
NCT03797547https://www.clinicaltrials.gov/study/NCT03797547?tab=tableNANANAThis is a multi centre, single arm, prospective observational phase 4 study in naive or pretreated patients with myopic neovascularization. The patients will be treated with intravitreal injections of Aflibercept following a real life protocol.
This sudy aims to evaluate the visual acuity during a 36 months period of time.
<![CDATA[
Studies
Study First Submitted Date | 2018-08-28 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2021-09-29 |
Start Month Year | June 22, 2018 |
Primary Completion Month Year | January 30, 2023 |
Verification Month Year | September 2021 |
Verification Date | 2021-09-30 |
Last Update Posted Date | 2021-09-29 |
Facilities
Sequence: | 200458242 |
Name | Chu de Poitiers |
City | Poitiers |
Country | France |
Browse Interventions
Sequence: | 96220658 | Sequence: | 96220659 | Sequence: | 96220660 | Sequence: | 96220661 | Sequence: | 96220662 | Sequence: | 96220663 | Sequence: | 96220664 |
Mesh Term | Aflibercept | Mesh Term | Angiogenesis Inhibitors | Mesh Term | Angiogenesis Modulating Agents | Mesh Term | Growth Substances | Mesh Term | Physiological Effects of Drugs | Mesh Term | Growth Inhibitors | Mesh Term | Antineoplastic Agents |
Downcase Mesh Term | aflibercept | Downcase Mesh Term | angiogenesis inhibitors | Downcase Mesh Term | angiogenesis modulating agents | Downcase Mesh Term | growth substances | Downcase Mesh Term | physiological effects of drugs | Downcase Mesh Term | growth inhibitors | Downcase Mesh Term | antineoplastic agents |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Conditions
Sequence: | 52277512 |
Name | Myopic Choroidal Neovascularisation |
Downcase Name | myopic choroidal neovascularisation |
Id Information
Sequence: | 40235504 |
Id Source | org_study_id |
Id Value | VIC |
Countries
Sequence: | 42653095 |
Name | France |
Removed | False |
Interventions
Sequence: | 52589568 |
Intervention Type | Other |
Name | AFLIBERCEPT |
Description | Patients will be treated following a real life protocol and according to the French recommendation |
Design Outcomes
Sequence: | 177770831 | Sequence: | 177770832 | Sequence: | 177770833 | Sequence: | 177770834 | Sequence: | 177770835 | Sequence: | 177770836 | Sequence: | 177770837 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | visual acuity measurement | Measure | visual acuity measurement in naive patient | Measure | visual acuity measurement after other treatment such as laser, pdt visudyneor other IVT treatment | Measure | pourcentage of patients who gain more than or equal of 15 letters | Measure | Anatomics parameters by oct | Measure | Anatomics parameters by color photographs | Measure | Anatomic parameters by fluoresceine angiography or angiography oct |
Time Frame | 6, 12, 24 and 36 months | Time Frame | 12, 24 and 36 months | Time Frame | 6, 12, 24 and 36 months | Time Frame | 6,12,24 and 36 months | Time Frame | 6, 12, 24 and 36 months | Time Frame | 6, 12, 24 and 36 months | Time Frame | 6, 12, 24 and 36 months |
Description | Efficacy measurement will be performed by mean change of "ETDRS" for Best Corrected Visual Acuity evaluation (ETDRS score at 4 meters) from baseline to 6, 12, 24 and 36 month after initation of treatment by aflibercept | Description | Efficacy measurement will be performed by mean change of "ETDRS" for Best corrected visual acuity evaluation from baseline to month 12, 24 and 36 after initation of treatment by aflibercept in naïve patients | Description | Efficacy measurement will be evaluated by mean change of "ETDRS" for Best corrected visual Acuity evaluation after initation of treatment by aflibercept after switch from other treatment such as laser, visudyne PDT or other IVT treatment, after 6, 12, 24 and 36 months of treatment with Eylea | Description | Efficacy measurement will be evaluated by pourcentage of patients who gain more than or equal of 15 letters at 6, 12, 24 and 36 months after initiation of treatment with aflibercept within naïve or after switch from other treatment such as laser, visudyne PDT or other IVT treatment, | Description | Evaluation of anatomic parameters will be perfomed after 6,12, and 24 and 36 months of treatment with Eylea based on OCT parameters :
On SD-OCT : Distance from CNV lesion to the fovea measured on the scan joining the fovea to the foveal edge of the mCNV Exudation assessed by presence of intraretinal cysts or subretinal fluid Central retinal thickness |
Description | On color retinal photographs:
Presence of retinal hemorrhage Presence of macular atrophy or lacquer cracks, |
Description | On fluoresceine angiography if deemed necessary by the investigator : diffusion during late phases On angiography OCT : neovascular network visualisation |
Browse Conditions
Sequence: | 193893016 | Sequence: | 193893017 | Sequence: | 193893018 | Sequence: | 193893019 | Sequence: | 193893020 | Sequence: | 193893021 | Sequence: | 193893022 | Sequence: | 193893023 | Sequence: | 193893024 |
Mesh Term | Choroidal Neovascularization | Mesh Term | Myopia | Mesh Term | Neovascularization, Pathologic | Mesh Term | Metaplasia | Mesh Term | Pathologic Processes | Mesh Term | Choroid Diseases | Mesh Term | Uveal Diseases | Mesh Term | Eye Diseases | Mesh Term | Refractive Errors |
Downcase Mesh Term | choroidal neovascularization | Downcase Mesh Term | myopia | Downcase Mesh Term | neovascularization, pathologic | Downcase Mesh Term | metaplasia | Downcase Mesh Term | pathologic processes | Downcase Mesh Term | choroid diseases | Downcase Mesh Term | uveal diseases | Downcase Mesh Term | eye diseases | Downcase Mesh Term | refractive errors |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48418698 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Poitiers University Hospital |
Eligibilities
Sequence: | 30827067 |
Sampling Method | Probability Sample |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 99 Years |
Healthy Volunteers | No |
Population | Active mCNV among: Naïve patients. Patients with previous history of laser photocoagulation or PDT, with no history of anti-VEGF. Patients with previous history of other anti-VEGF treatments.including ranibizumab or bevacizumab, with sustaining mCNV activity, who did not receive injection since the last 3 month |
Criteria | Inclusion Criteria:
Man or woman aged 18 years and more under reliable method of contraception for woman with childbearing potenteial (hormonal or any intrauterine devices). • Patients naïve or Patients pretreated with previous history of laser photocoagulation or PDT or by other anti-VEGF treatments who did not receive injection since the last 3 month with OCT or angiography examination Exclusion Criteria: Treatment with an anti VEGF administrated by intravitreal injection within 1 months prior to baseline in the study eye. |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254123813 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2018 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 99 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 6 |
Designs
Sequence: | 30572997 |
Observational Model | Cohort |
Time Perspective | Prospective |
Responsible Parties
Sequence: | 28939419 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797534
2019-02-01
https://zephyrnet.com/?p=NCT03797534
NCT03797534https://www.clinicaltrials.gov/study/NCT03797534?tab=tableNANANAThe purpose of this study is to explore the individualized administration model of warfarin suitable for Chinese people, and provide a scientific reference for the use of warfarin to Chinese people.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-06 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-15 |
Start Month Year | February 1, 2019 |
Primary Completion Month Year | January 1, 2022 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-15 |
Detailed Descriptions
Sequence: | 20716306 |
Description | About 600 patients with VKORC1 and CYP2C9 gene mutations were included in the treatment of warfarin anticoagulant therapy. The main indications include valve replacement, atrial fibrillation, pulmonary embolism, etc., randomly divided into 2 groups, respectively, the control group (that is, the use of fixed-dose group), Bayesian-model group, the use of single-blind treatment method, to evaluate the number of major adverse events, TTR and INR adjustments in patients between different groups after three months of taking warfarin, and then to explore the individualized drug use model of warfarin suitable for Chinese population.
In the Bayesian group, according to the genotype of VKORC1 and CYP2C9, the stable dose was calculated by the dose prediction model of Bayesian, and the first three drugs were taken at this dose, and then adjusted to the actual stable dose according to the change of INR. Meanwhile, the control group was administered according to the traditional way, that is, the initial dose is 2.5 or 3mg/d and is gradually adjusted to a stable dose according to changes of INR. The monitoring frequency of INR is: once a day from the beginning of the drug to the time of discharge, once a week after discharge, and once a month after the stable dose is obtained. Detailed records of the number of days to reach a stable dose, the INR value and the occurrence of side effects and time are documented. The concrete steps are as follows: clinicians to judge the standard of the selection criteria; Finally,according to the outcome parameters,statistical analysis were performed with SPSS 11.5 software. A value of P < 0.05 was considered statistically significant. |
Facilities
Sequence: | 200053337 |
Status | Recruiting |
Name | the Department of Cardiovascular Surgery |
City | FuZhou |
State | Fujian |
Zip | 350001 |
Country | China |
Facility Contacts
Sequence: | 28097566 | Sequence: | 28097567 |
Facility Id | 200053337 | Facility Id | 200053337 |
Contact Type | primary | Contact Type | backup |
Name | Liang-Wan Chen, M.D Ph.D | Name | Jin-Hua Zhang, Ph.D |
343983217@qq.com | pollyzhang2006@126.com | ||
Phone | 86 13358255333 | Phone | 86 13609532263 |
Conditions
Sequence: | 52156524 |
Name | Heart Valve Prosthesis |
Downcase Name | heart valve prosthesis |
Id Information
Sequence: | 40148230 |
Id Source | org_study_id |
Id Value | CLW2018WA |
Countries
Sequence: | 42557763 |
Name | China |
Removed | False |
Design Groups
Sequence: | 55577929 | Sequence: | 55577930 |
Group Type | No Intervention | Group Type | Experimental |
Title | Standard anticoagulant group | Title | Bayesian model group |
Interventions
Sequence: | 52472030 |
Intervention Type | Other |
Name | dose regime |
Description | The initial dose of the experimental group will be calculated by the Bayesian model. |
Keywords
Sequence: | 79848137 | Sequence: | 79848138 |
Name | warfarin | Name | gene |
Downcase Name | warfarin | Downcase Name | gene |
Design Outcomes
Sequence: | 177328074 | Sequence: | 177328075 | Sequence: | 177328072 | Sequence: | 177328076 | Sequence: | 177328073 | Sequence: | 177328068 | Sequence: | 177328069 | Sequence: | 177328070 | Sequence: | 177328071 | Sequence: | 177328077 | Sequence: | 177328078 | Sequence: | 177328079 |
Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | The time required from the beginning of treatment to the stable dose; | Measure | The percentage of time below the target INR range; | Measure | Percentage of time in therapeutic range | Measure | The percentage of time above the target INR range; | Measure | The time required to reach the treatment target INR for the first time; | Measure | excessive anticoagulant time ratio | Measure | The occurrence of primary bleeding events | Measure | The occurance of secondary bleeding events | Measure | The occurrence of thrombosis events | Measure | The number of dose adjustments and the number of INR measured during the first month of treatment; | Measure | The proportion of patients in each group receiving a stable dose after follow-up; | Measure | The proportion of patients in each group having side effects after follow-up |
Time Frame | 3 months postoperatively | Time Frame | 3 months postoperatively | Time Frame | 3 months, 6 months, 12 months postoperatively | Time Frame | 3 months postoperatively | Time Frame | 3 months postoperatively | Time Frame | 3 months postoperatively | Time Frame | 3 months postoperatively | Time Frame | 3 months postoperatively | Time Frame | 3 months postoperatively | Time Frame | 3 months postoperatively | Time Frame | 3 months postoperatively | Time Frame | 3 months postoperatively |
Description | INR>3,INR>4 | Description | gastrointestinal hemorrhage, intracerebral hemorrhage,etc | Description | nasal bleeding, skin stasis,etc | Description | ischemic stroke, deep vein thrombosis,etc |
Sponsors
Sequence: | 48306103 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Fujian Medical University |
Design Group Interventions
Sequence: | 68130893 |
Design Group Id | 55577930 |
Intervention Id | 52472030 |
Eligibilities
Sequence: | 30757371 |
Gender | All |
Minimum Age | 14 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Age > 14 years old; Exclusion Criteria: Severe liver dysfunction (ChildPugh ≥ 10); |
Adult | True |
Child | True |
Older Adult | True |
Calculated Values
Sequence: | 254228093 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 14 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 4 |
Number Of Secondary Outcomes To Measure | 8 |
Designs
Sequence: | 30503596 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Supportive Care |
Time Perspective | |
Masking | Double |
Subject Masked | True |
Caregiver Masked | True |
Responsible Parties
Sequence: | 28869874 |
Responsible Party Type | Principal Investigator |
Name | Liang-Wan Chen MD |
Title | The director of the department of cardiovascular surgery |
Affiliation | Fujian Medical University |
Study References
Sequence: | 52049419 | Sequence: | 52049420 | Sequence: | 52049421 | Sequence: | 52049422 | Sequence: | 52049423 | Sequence: | 52049424 |
Pmid | 18305455 | Pmid | 19228618 | Pmid | 25889768 | Pmid | 24251363 | Pmid | 24251361 | Pmid | 25628141 |
Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background |
Citation | Gage BF, Eby C, Johnson JA, Deych E, Rieder MJ, Ridker PM, Milligan PE, Grice G, Lenzini P, Rettie AE, Aquilante CL, Grosso L, Marsh S, Langaee T, Farnett LE, Voora D, Veenstra DL, Glynn RJ, Barrett A, McLeod HL. Use of pharmacogenetic and clinical factors to predict the therapeutic dose of warfarin. Clin Pharmacol Ther. 2008 Sep;84(3):326-31. doi: 10.1038/clpt.2008.10. Epub 2008 Feb 27. Erratum In: Clin Pharmacol Ther. 2008 Sep;84(3):430. | Citation | International Warfarin Pharmacogenetics Consortium; Klein TE, Altman RB, Eriksson N, Gage BF, Kimmel SE, Lee MT, Limdi NA, Page D, Roden DM, Wagner MJ, Caldwell MD, Johnson JA. Estimation of the warfarin dose with clinical and pharmacogenetic data. N Engl J Med. 2009 Feb 19;360(8):753-64. doi: 10.1056/NEJMoa0809329. Erratum In: N Engl J Med. 2009 Oct 15;361(16):1613. Dosage error in article text. | Citation | Hamberg AK, Hellman J, Dahlberg J, Jonsson EN, Wadelius M. A Bayesian decision support tool for efficient dose individualization of warfarin in adults and children. BMC Med Inform Decis Mak. 2015 Feb 7;15:7. doi: 10.1186/s12911-014-0128-0. | Citation | Pirmohamed M, Burnside G, Eriksson N, Jorgensen AL, Toh CH, Nicholson T, Kesteven P, Christersson C, Wahlstrom B, Stafberg C, Zhang JE, Leathart JB, Kohnke H, Maitland-van der Zee AH, Williamson PR, Daly AK, Avery P, Kamali F, Wadelius M; EU-PACT Group. A randomized trial of genotype-guided dosing of warfarin. N Engl J Med. 2013 Dec 12;369(24):2294-303. doi: 10.1056/NEJMoa1311386. Epub 2013 Nov 19. | Citation | Kimmel SE, French B, Kasner SE, Johnson JA, Anderson JL, Gage BF, Rosenberg YD, Eby CS, Madigan RA, McBane RB, Abdel-Rahman SZ, Stevens SM, Yale S, Mohler ER 3rd, Fang MC, Shah V, Horenstein RB, Limdi NA, Muldowney JA 3rd, Gujral J, Delafontaine P, Desnick RJ, Ortel TL, Billett HH, Pendleton RC, Geller NL, Halperin JL, Goldhaber SZ, Caldwell MD, Califf RM, Ellenberg JH; COAG Investigators. A pharmacogenetic versus a clinical algorithm for warfarin dosing. N Engl J Med. 2013 Dec 12;369(24):2283-93. doi: 10.1056/NEJMoa1310669. Epub 2013 Nov 19. | Citation | Li X, Yang J, Wang X, Xu Q, Zhang Y, Yin T. Clinical benefits of pharmacogenetic algorithm-based warfarin dosing: meta-analysis of randomized controlled trials. Thromb Res. 2015 Apr;135(4):621-9. doi: 10.1016/j.thromres.2015.01.018. Epub 2015 Jan 17. |
]]>
https://zephyrnet.com/NCT03797521
2018-12-19
https://zephyrnet.com/?p=NCT03797521
NCT03797521https://www.clinicaltrials.gov/study/NCT03797521?tab=tableNANANAThe purpose of this study is to explore the safety, tolerability and activity of SXC-2023 when dosed for 6 weeks versus placebo in adult patients with moderate to severe Trichotillomania.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-02 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2021-10-28 |
Start Month Year | December 19, 2018 |
Primary Completion Month Year | December 2, 2019 |
Verification Month Year | October 2021 |
Verification Date | 2021-10-31 |
Last Update Posted Date | 2021-10-28 |
Detailed Descriptions
Sequence: | 20787714 |
Description | This is a Phase 2, multicenter, double-blind, placebo-controlled, parallel-group study consisting of a screening period of up to 40 days, a 6 week randomized double-blind treatment period, followed by an up to 2 week safety follow-up period after the last dose of study medication.
Patients will be randomized to one of four treatment groups. Patients will participate for a total of up to 10 weeks, including screening, the 6-week treatment period and follow-up. |
Facilities
Sequence: | 200656939 | Sequence: | 200656940 | Sequence: | 200656941 | Sequence: | 200656942 | Sequence: | 200656943 | Sequence: | 200656944 | Sequence: | 200656945 | Sequence: | 200656946 | Sequence: | 200656947 | Sequence: | 200656948 | Sequence: | 200656949 | Sequence: | 200656950 | Sequence: | 200656951 |
Name | CNRI- Los Angeles | Name | Artemis Institute for Clinical Research | Name | Behavioral Clinical Research | Name | iResearch Atlanta | Name | Univ of Chicago | Name | Lake Charles Clinical Trials | Name | Massachusetts General Hospital | Name | Integrative Clinical Trials, LLC | Name | Finger Lakes Clinical Research | Name | Insight Clinical Trials, LLC | Name | IPS Research Company | Name | Carolina Clinical Trials, Inc | Name | Northwest Clinical Research Center |
City | Pico Rivera | City | Riverside | City | North Miami | City | Decatur | City | Chicago | City | Lake Charles | City | Boston | City | Brooklyn | City | Rochester | City | Shaker Heights | City | Oklahoma City | City | Charleston | City | Bellevue |
State | California | State | California | State | Florida | State | Georgia | State | Illinois | State | Louisiana | State | Massachusetts | State | New York | State | New York | State | Ohio | State | Oklahoma | State | South Carolina | State | Washington |
Zip | 90662 | Zip | 92503 | Zip | 33161 | Zip | 30030 | Zip | 60637 | Zip | 70629 | Zip | 02114 | Zip | 11229 | Zip | 14618 | Zip | 44122 | Zip | 73103 | Zip | 29407 | Zip | 98007 |
Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States |
Conditions
Sequence: | 52340163 |
Name | Trichotillomania |
Downcase Name | trichotillomania |
Id Information
Sequence: | 40279586 |
Id Source | org_study_id |
Id Value | PRO-201 |
Countries
Sequence: | 42699712 |
Name | United States |
Removed | False |
Design Groups
Sequence: | 55781354 | Sequence: | 55781355 | Sequence: | 55781356 | Sequence: | 55781357 |
Group Type | Experimental | Group Type | Experimental | Group Type | Experimental | Group Type | Placebo Comparator |
Title | SXC-2023 50mg QD | Title | SXC-2023 200mg QD | Title | SXC-2023 800mg QD | Title | Matching Placebo QD |
Description | SXC-2023 50mg dosed once daily for 6 weeks | Description | SXC-2023 200mg dosed once daily for 6 weeks | Description | SXC-2023 800mg dosed once daily for 6 weeks | Description | Matching Placebo dosed once daily for 6 weeks |
Interventions
Sequence: | 52650881 | Sequence: | 52650882 |
Intervention Type | Drug | Intervention Type | Drug |
Name | SXC-2023 | Name | Placebo |
Description | SXC-2023 oral capsules | Description | Matching Placebo oral capsules |
Keywords
Sequence: | 80102046 | Sequence: | 80102047 | Sequence: | 80102048 |
Name | Promentis Pharmaceuticals | Name | TTM | Name | SXC-2023 |
Downcase Name | promentis pharmaceuticals | Downcase Name | ttm | Downcase Name | sxc-2023 |
Design Outcomes
Sequence: | 178002910 | Sequence: | 178002911 | Sequence: | 178002912 | Sequence: | 178002913 | Sequence: | 178002914 | Sequence: | 178002915 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Explore the incidence of treatment-emergent adverse events in adults with moderate to severe TTM | Measure | Change from baseline hairpulling frequency and severity through 6 weeks | Measure | Change from baseline hairpulling frequency and severity through 6 weeks | Measure | Change from baseline hairpulling frequency and severity through 6 weeks | Measure | Change from baseline hairpulling frequency and severity daily through 6 weeks | Measure | Preliminary psychometric evidence of the Trichotillomania Symptom Diary (TSD) will be assessed |
Time Frame | Up to 7 weeks | Time Frame | Up to 7 weeks | Time Frame | Up to 7 weeks | Time Frame | Up to 7 weeks | Time Frame | Up to 7 weeks | Time Frame | Up to 7 weeks |
Description | Safety and tolerability assessed using the frequency of subjects with serious adverse events, adverse events leading to discontinuation, and adverse events judged to be related to study medication. | Description | Improvement will be assessed using the different measurement parameters of all scales using scales such as the Massachusetts General Hospital Hairpulling scale (MGH-HPS) | Description | Improvement will be assessed using the different measurement parameters of all scales using scales such as the Clinical Global Impression of Severity and Change (CGI-S/C) | Description | Improvement will be assessed using the different measurement parameters of all scales using scales such as the Patient Global Impression of Status and Change (PGI-S/C) | Description | Improvement will be assessed using the different measurement parameters of all scales using scales such as the Trichotillomania Symptom Diary (TSD) | Description | The reliability, validity and responsiveness of the newly developed TSD assessment will be assessed at the item level. |
Browse Conditions
Sequence: | 194130239 | Sequence: | 194130240 | Sequence: | 194130241 |
Mesh Term | Trichotillomania | Mesh Term | Disruptive, Impulse Control, and Conduct Disorders | Mesh Term | Mental Disorders |
Downcase Mesh Term | trichotillomania | Downcase Mesh Term | disruptive, impulse control, and conduct disorders | Downcase Mesh Term | mental disorders |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48477246 |
Agency Class | INDUSTRY |
Lead Or Collaborator | lead |
Name | Promentis Pharmaceuticals, Inc. |
Overall Officials
Sequence: | 29375117 |
Role | Study Director |
Name | Dean Brostowin |
Affiliation | Promentis Pharmaceuticals |
Design Group Interventions
Sequence: | 68378289 | Sequence: | 68378290 | Sequence: | 68378291 | Sequence: | 68378292 |
Design Group Id | 55781355 | Design Group Id | 55781354 | Design Group Id | 55781356 | Design Group Id | 55781357 |
Intervention Id | 52650881 | Intervention Id | 52650881 | Intervention Id | 52650881 | Intervention Id | 52650882 |
Eligibilities
Sequence: | 30863199 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 45 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria
Adult, female or male, 18-45 years of age, inclusive at screening. Diagnosis of current TTM based on Diagnostic and Statistical Manual of Mental Disorders, fifth edition (DSM-5) criteria and confirmed using the clinician-administered MINI-TTM. In addition, subjects should: Have a history of TTM for at least one year For a female of childbearing potential: either be sexually inactive (abstinent as a life style) for 28 days prior to the first dosing and throughout the study or be using one of the following acceptable birth control options: Oral contraception for at least 3 months prior to the first dosing along with either a physical (e.g., condom, diaphragm) or a chemical (e.g., spermicide) barrier method from the time of screening and throughout the study In addition, female subjects of childbearing potential will be advised to remain sexually inactive or to keep the same birth control method for at least 30 days following the last dose. Female of non childbearing potential: must have undergone one of the following sterilization procedures, at least 6 months prior to the first dose: hysteroscopic sterilization; Exclusion Criteria: Females who are pregnant or breastfeeding or intend to become pregnant during the study period or within 30 days of the final dose of study drug. Subjects with any of the following: Any psychiatric hospitalizations in the past year, |
Adult | True |
Child | False |
Older Adult | False |
Calculated Values
Sequence: | 253933123 |
Number Of Facilities | 13 |
Registered In Calendar Year | 2019 |
Actual Duration | 11 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | False |
Minimum Age Num | 18 |
Maximum Age Num | 45 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 5 |
Designs
Sequence: | 30609022 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Quadruple |
Masking Description | Double-blind, Placebo-controlled Study |
Subject Masked | True |
Caregiver Masked | True |
Investigator Masked | True |
Outcomes Assessor Masked | True |
Provided Documents
Sequence: | 2592323 | Sequence: | 2592324 |
Document Type | Study Protocol | Document Type | Statistical Analysis Plan |
Has Protocol | True | Has Protocol | False |
Has Icf | False | Has Icf | False |
Has Sap | False | Has Sap | True |
Document Date | 2019-06-25 | Document Date | 2019-06-25 |
Url | https://ClinicalTrials.gov/ProvidedDocs/21/NCT03797521/Prot_000.pdf | Url | https://ClinicalTrials.gov/ProvidedDocs/21/NCT03797521/SAP_001.pdf |
Responsible Parties
Sequence: | 28975560 |
Responsible Party Type | Sponsor |
Study References
Sequence: | 52245353 |
Pmid | 34582562 |
Reference Type | derived |
Citation | Hoffman J, Williams T, Rothbart R, Ipser JC, Fineberg N, Chamberlain SR, Stein DJ. Pharmacotherapy for trichotillomania. Cochrane Database Syst Rev. 2021 Sep 28;9(9):CD007662. doi: 10.1002/14651858.CD007662.pub3. |
]]>
https://zephyrnet.com/NCT03797508
2018-12-01
https://zephyrnet.com/?p=NCT03797508
NCT03797508https://www.clinicaltrials.gov/study/NCT03797508?tab=tablemohamed k abdelwahab, masterm.k.ali1987@gmail.com01000849822Threatened miscarriage occurs in about one-fifth of pregnancies with an estimated miscarriage rate of 3-16% after successful demonstration of fetal cardiac activity. Various biochemical markers have been studied previously to predict the outcome of threatened miscarriage; However, the results have been conflicting. Several studies have documented that a slow embryonic heart rate at 6.0-7.0 Weeks’ gestation is associated with a high rate of first trimester fetal demise.
our aim: To evaluate the accuracy of ultrasound findings in comparison to serum CA125 and progesterone in predicting fetal demise in cases of first trimester threatened miscarriage.
Will this pregnancy be continued after the first trimester or not?
<![CDATA[
Studies
Study First Submitted Date | 2019-01-06 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-02-05 |
Start Month Year | December 1, 2018 |
Primary Completion Month Year | May 31, 2019 |
Verification Month Year | February 2019 |
Verification Date | 2019-02-28 |
Last Update Posted Date | 2019-02-05 |
Detailed Descriptions
Sequence: | 20721682 |
Description | we are comparing between the accuracy of vaginal ultra sound versus serum progesterone level and serum CA 125 level in predicting of fetal demise in cases of threatened miscarriage three vaginal ultrasounds will be done ) the first one will be done at six to eight weeks of pregnancy to the patients who fulfill the criteria in this us we will make sure that the cardiac pulsations are present and measure the following:
the fetal heart rate, C) the third one will be at the end of first trimester (13 weeks) to ensure fetal viability. . embryonic bradycardia and absence of yolk sac or smaller yolk sac than expected for any given gestational age are prognostic factors of poor pregnancy outcome in the first 12 weeks of pregnancy women with small for age gestational sac are more prone to have miscarriage we will do laboratory investigation in the form of A) Serum progesterone: low maternal P levels have been useful in predicting spontaneous abortion in threatened pregnancies with a sensitivity of 80% (<10 ng /mL) so, this will be our cutoff value. B) Serum CA 125 :we will take a level of 51.5 as cut off value.this is the upper level of normal we will do them once when the patient presents to us. |
Facilities
Sequence: | 200108804 |
Status | Recruiting |
Name | Ain Shams University |
City | Cairo |
Country | Egypt |
Browse Interventions
Sequence: | 96050400 | Sequence: | 96050401 | Sequence: | 96050402 | Sequence: | 96050403 | Sequence: | 96050404 |
Mesh Term | Progesterone | Mesh Term | Progestins | Mesh Term | Hormones | Mesh Term | Hormones, Hormone Substitutes, and Hormone Antagonists | Mesh Term | Physiological Effects of Drugs |
Downcase Mesh Term | progesterone | Downcase Mesh Term | progestins | Downcase Mesh Term | hormones | Downcase Mesh Term | hormones, hormone substitutes, and hormone antagonists | Downcase Mesh Term | physiological effects of drugs |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Conditions
Sequence: | 52171371 |
Name | Abortion Threatened |
Downcase Name | abortion threatened |
Id Information
Sequence: | 40158710 |
Id Source | org_study_id |
Id Value | us laboratory miscarriage |
Countries
Sequence: | 42569046 |
Name | Egypt |
Removed | False |
Design Groups
Sequence: | 55593301 |
Group Type | Other |
Title | threatened miscarriage |
Description | ultrasound ,CA125,progesterone |
Interventions
Sequence: | 52485595 |
Intervention Type | Diagnostic Test |
Name | ultrasound |
Description | To evaluate the accuracy of ultrasound findings in comparison to serum CA125and progesterone in predicting fetal demise in cases of first trimester threatened miscarriage. |
Design Outcomes
Sequence: | 177379282 |
Outcome Type | primary |
Measure | ultra sound |
Time Frame | the 12th week of gestation |
Description | presence of fetal heart rate |
Browse Conditions
Sequence: | 193487201 | Sequence: | 193487202 | Sequence: | 193487203 | Sequence: | 193487204 | Sequence: | 193487205 |
Mesh Term | Abortion, Spontaneous | Mesh Term | Abortion, Threatened | Mesh Term | Pregnancy Complications | Mesh Term | Female Urogenital Diseases and Pregnancy Complications | Mesh Term | Urogenital Diseases |
Downcase Mesh Term | abortion, spontaneous | Downcase Mesh Term | abortion, threatened | Downcase Mesh Term | pregnancy complications | Downcase Mesh Term | female urogenital diseases and pregnancy complications | Downcase Mesh Term | urogenital diseases |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48319405 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Ain Shams University |
Overall Officials
Sequence: | 29285413 |
Role | Principal Investigator |
Name | amany a mahmoud |
Affiliation | Ain Shams University |
Central Contacts
Sequence: | 12008911 |
Contact Type | primary |
Name | mohamed k abdelwahab, master |
Phone | 01000849822 |
m.k.ali1987@gmail.com | |
Phone Extension | 002 |
Role | Contact |
Design Group Interventions
Sequence: | 68149273 |
Design Group Id | 55593301 |
Intervention Id | 52485595 |
Eligibilities
Sequence: | 30765419 |
Gender | Female |
Minimum Age | 20 Years |
Maximum Age | 35 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Singleton Pregnancy. Exclusion Criteria: Patients with recurrent miscarriage or pregnancy of unknown location (PUL). Patients had ovulation induction medications or on progesterone treatment. |
Adult | True |
Child | False |
Older Adult | False |
Calculated Values
Sequence: | 253889281 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 20 |
Maximum Age Num | 35 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Designs
Sequence: | 30511585 |
Allocation | N/A |
Intervention Model | Single Group Assignment |
Observational Model | |
Primary Purpose | Other |
Time Perspective | |
Masking | None (Open Label) |
Intervention Other Names
Sequence: | 26673784 | Sequence: | 26673785 |
Intervention Id | 52485595 | Intervention Id | 52485595 |
Name | progesterone | Name | CA125 |
Responsible Parties
Sequence: | 28877880 |
Responsible Party Type | Principal Investigator |
Name | amany abdel monem mahmoud |
Title | Egypt Cairo |
Affiliation | Ain Shams University |
]]>
https://zephyrnet.com/NCT03797495
2018-12-18
https://zephyrnet.com/?p=NCT03797495
NCT03797495https://www.clinicaltrials.gov/study/NCT03797495?tab=tableCharles Nakar, MDcnakar@ihtc.org317-871-0000This is an Investigator initiated retrospective and prospective single cohort study. The study will utilize an international registry and develop a specimen biobank to provide an improved understanding of the natural history of hyposplasminogenemia, to elucidate the heterogeneity of phenotypic expression, identify markers to predict disease course, and inform improved therapeutic modalities
<![CDATA[
Studies
Study First Submitted Date | 2018-12-28 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2023-06-18 |
Start Month Year | December 18, 2018 |
Primary Completion Month Year | March 8, 2027 |
Verification Month Year | June 2023 |
Verification Date | 2023-06-30 |
Last Update Posted Date | 2023-06-18 |
Detailed Descriptions
Sequence: | 20845122 |
Description | The aims of this study are to:
Define PLGD natural history in a large cohort of individuals with hypoplasminogenemia and their first-degree family members. The project will be international in scope with two collaborating centers that have created and will collect the subject data and samples. In North/Central/South America, the Indiana Hemophilia & Thrombosis Center (IHTC) will serve as the primary site while University of Milan will serve as the center for all other sites. The database is housed at the University of Milan, Italy. Study population will include males and females affected with hyposplasminogenemia of any age. Both one-year retrospective and three-year prospective data will be collected on an international cohort of 100 affected individuals and their first degree family members (parents, siblings; total estimated study population ~500). Study sample analysis, except for urine analyses, will be centralized and performed in Italy; the plasminogen antibody analysis will be batched for analysis, and the urine analyses will be performed locally. A sample biorepository will be created and ultimately housed in Italy. The study will provide testing for plasminogen activity and antigen, plasminogen genetic analysis, polymorphisms in genes that impact plasminogen expression and fibrinolysis, and global hemostatic assays. In addition, stored samples will be used for further testing and analyses to potentially include whole genome sequencing to further identify plasminogen genetic mutations as needed and to investigate other genetic modifiers of disease expression. An exploratory aim includes investigating the potential relationship with streptococcal strains and altered plasminogen products. The study period will be 3 years for each enrolled subject. In-person visits will be conducted and samples for analysis will be collected at baseline and at end of study. Interval follow-up will be performed every 6 months by telephone. data will be collected at unscheduled visits that are performed for clinical need at the treating physician's discretion. |
Facilities
Sequence: | 201223995 | Sequence: | 201223996 | Sequence: | 201223997 | Sequence: | 201223998 | Sequence: | 201223999 | Sequence: | 201224000 | Sequence: | 201224001 | Sequence: | 201224002 | Sequence: | 201224003 | Sequence: | 201224004 | Sequence: | 201224005 | Sequence: | 201224006 | Sequence: | 201224007 | Sequence: | 201224008 | Sequence: | 201224009 |
Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting |
Name | Indiana Hemophila @Thrombosis Center | Name | Hemophilia Center of Western Pennsylvania | Name | Vanderbilt Children's Hematology-Oncology | Name | Cook Children's Medical Center | Name | The University of Texas Health Science Center at Houston | Name | Hospital Britanico Buenos Aires | Name | Murdoch Children's Research Institute, The Royal Children's Hospital | Name | University of Saskatchewan | Name | Angelo Bianchi Bonomi Hemophilia and Thrombosis Center, | Name | University Hospital of Padova | Name | Faculty of Medicine, Chiang Mai University | Name | Dokuz Eylul University pediatric Pulmonology, Allergy and Clinical Immunology | Name | Istanbul Üniversitesi Onkoloji Enstitüsü | Name | Istanbul University Cerrahpsasa, Cerrahpsasa Medical Faculty Pediatric Hematology and Oncology Department | Name | Yuzuncu Yil University Faculty of Medicine Department of Ophthalmology |
City | Indianapolis | City | Pittsburgh | City | Nashville | City | Fort Worth | City | Houston | City | Buenos Aires | City | Melbourne | City | Saskatoon | City | Milano | City | Padua | City | Chiang Mai | City | Izmir | City | Istanbul | City | Istanbul | City | Van |
State | Indiana | State | Pennsylvania | State | Tennessee | State | Texas | State | Texas | State | Victoria | State | Balçova | ||||||||||||||||
Zip | 46260 | Zip | 15213 | Zip | 37232 | Zip | 76104 | Zip | 77030 | Zip | C1280 | Zip | 3052 | Zip | SK S7N 0W8 | Zip | 20122 | Zip | 35100 | Zip | 50200 | Zip | 35330 | Zip | 34093 | Zip | 34098 | Zip | 65040 |
Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | Argentina | Country | Australia | Country | Canada | Country | Italy | Country | Italy | Country | Thailand | Country | Turkey | Country | Turkey | Country | Turkey | Country | Turkey |
Facility Contacts
Sequence: | 28273404 | Sequence: | 28273405 | Sequence: | 28273406 | Sequence: | 28273407 | Sequence: | 28273408 | Sequence: | 28273409 | Sequence: | 28273410 | Sequence: | 28273411 | Sequence: | 28273412 | Sequence: | 28273413 | Sequence: | 28273414 | Sequence: | 28273415 | Sequence: | 28273416 | Sequence: | 28273417 | Sequence: | 28273418 | Sequence: | 28273419 | Sequence: | 28273420 | Sequence: | 28273421 | Sequence: | 28273422 | Sequence: | 28273423 | Sequence: | 28273424 | Sequence: | 28273425 | Sequence: | 28273426 | Sequence: | 28273427 | Sequence: | 28273428 |
Facility Id | 201223995 | Facility Id | 201223995 | Facility Id | 201223996 | Facility Id | 201223996 | Facility Id | 201223997 | Facility Id | 201223997 | Facility Id | 201223998 | Facility Id | 201223998 | Facility Id | 201223999 | Facility Id | 201223999 | Facility Id | 201224000 | Facility Id | 201224000 | Facility Id | 201224001 | Facility Id | 201224001 | Facility Id | 201224002 | Facility Id | 201224002 | Facility Id | 201224003 | Facility Id | 201224004 | Facility Id | 201224004 | Facility Id | 201224005 | Facility Id | 201224006 | Facility Id | 201224007 | Facility Id | 201224008 | Facility Id | 201224008 | Facility Id | 201224009 |
Contact Type | primary | Contact Type | backup | Contact Type | primary | Contact Type | backup | Contact Type | primary | Contact Type | backup | Contact Type | primary | Contact Type | backup | Contact Type | primary | Contact Type | backup | Contact Type | primary | Contact Type | backup | Contact Type | primary | Contact Type | backup | Contact Type | primary | Contact Type | backup | Contact Type | primary | Contact Type | primary | Contact Type | backup | Contact Type | primary | Contact Type | primary | Contact Type | primary | Contact Type | primary | Contact Type | backup | Contact Type | primary |
Name | Neelam Thukral, CCRC | Name | Charles Nakar, MD | Name | Frederico Xavier, MD | Name | Debbie Vehec | Name | Delia Darst | Name | Heather McDaniel, MD, MSCI | Name | Heather Urbanek | Name | Marcela Torres, MD | Name | Katherine Addy, RN, BSN, MPH | Name | Nidra Rodriguez, MD | Name | Jhon A Avila, MD | Name | Jose M Ceresetto, MD | Name | Paul Monagle, MD | Name | Jodi Hislop, RN | Name | Sarah Tehseen, MBBS, MSc. FRCPC | Name | Rashmi Nagaraj | Name | Marzia Menegatti, PhD | Name | Maria Teresa Sartori, MD | Name | C. Dalla Porta, MD | Name | Rungrote Natesirinilkul, MD | Name | Serdar Al, MD | Name | Basak Koc, MD | Name | Ayse Gonca Kacar, MD | Name | Tulin Celkan, MD | Name | Muhammed Batur, MD |
nthukral@ihtc.org | cnakar@ihtc.org | fxavier@hmc.psu.edu | dvehec@vitalant.org | delia.h.darst@vumc.org | heather.mcdaniel@vumc.org | Heather.Urbanek@cookchildrens.org | marcela.torres@cookchildrens.org | Katherine.E.Addy@uth.tmc.edu | Nidra.I.Rodriguez@uth.tmc.edu | jaavilar@gmail.com | jceresetto@intramed.net | paul.monagle@rch.org.au | jodi.hislop@rch.org.au | Sarah.Tehseen@saskhealthauthority.ca | rashmi.nagaraj@usask.ca | marzia.menegatti@guest.unimi.it | mtsart@unipd.it | cesare.dallaporta@gmail.com | rungrote.n@cmu.ac.th | drserdaral@gmail.com | s_basakkoc@hotmail.com | goncakacar@gmail.com | tirajecelkan@yahoo.com | muhammedbatur@gmail.com | |||||||||||||||||||||||||
Phone | 317-871-0000 | Phone | 317-871-0000 | Phone | 412-209-7411 | Phone | 412-209-7564 | Phone | 615-343-7190 | Phone | 615 936 1762 | Phone | 682-885-1244 | Phone | 682 885 4007 | Phone | 713-500-8352 | Phone | 713 500 8360 | Phone | 549 114 187 9723 | Phone | 541 143 041 081 | Phone | 61 3 9936-6330 | Phone | 61 3 9936-6330 | Phone | 639 998 3972 | Phone | 306-978-8306 | Phone | +39 – 02/50320727 | Phone | 3334530450 | Phone | 39 049 821 1111 | Phone | 66 2 201 1749 | Phone | 905336510797 | Phone | 90 5326003027 | Phone | 505 259 1229 | Phone | 532 57 60723 | Phone | 904 322 150 473 |
Phone Extension | 373 | Phone Extension | 6030 |
Facility Investigators
Sequence: | 18434231 | Sequence: | 18434232 | Sequence: | 18434233 | Sequence: | 18434234 | Sequence: | 18434235 | Sequence: | 18434236 | Sequence: | 18434237 | Sequence: | 18434238 | Sequence: | 18434239 | Sequence: | 18434240 | Sequence: | 18434241 | Sequence: | 18434242 | Sequence: | 18434243 | Sequence: | 18434244 | Sequence: | 18434245 | Sequence: | 18434246 |
Facility Id | 201223995 | Facility Id | 201223995 | Facility Id | 201223997 | Facility Id | 201223998 | Facility Id | 201223999 | Facility Id | 201224000 | Facility Id | 201224000 | Facility Id | 201224001 | Facility Id | 201224002 | Facility Id | 201224003 | Facility Id | 201224004 | Facility Id | 201224005 | Facility Id | 201224006 | Facility Id | 201224007 | Facility Id | 201224008 | Facility Id | 201224009 |
Role | Principal Investigator | Role | Sub-Investigator | Role | Principal Investigator | Role | Principal Investigator | Role | Principal Investigator | Role | Principal Investigator | Role | Sub-Investigator | Role | Principal Investigator | Role | Principal Investigator | Role | Principal Investigator | Role | Principal Investigator | Role | Principal Investigator | Role | Principal Investigator | Role | Principal Investigator | Role | Principal Investigator | Role | Principal Investigator |
Name | Amy D Shapiro, MD | Name | Charles Nakar, MD | Name | Heather McDaniel, MD, MSCI | Name | Marcela Torres, MD | Name | Nidra Rodriguez, MD | Name | Jose M Ceresetto, MD | Name | Jhon A Avila, MD | Name | Paul Monagle, MD | Name | Sarah Tehseen, MBBS, MSc. FRCPC | Name | Flora Peyvandi, MD,PhD | Name | Maria Teresa Sartori, MD | Name | Rungrote Natesirinilkul, MD | Name | Serdar Al, MD | Name | Basak Koc, MD | Name | Tulin Celkan, MD | Name | Muhammed Batur, MD |
Conditions
Sequence: | 52488208 |
Name | Plasminogen Deficiency |
Downcase Name | plasminogen deficiency |
Id Information
Sequence: | 40385176 |
Id Source | org_study_id |
Id Value | HISTORY |
Countries
Sequence: | 42820903 | Sequence: | 42820904 | Sequence: | 42820905 | Sequence: | 42820906 | Sequence: | 42820907 | Sequence: | 42820908 | Sequence: | 42820909 |
Name | United States | Name | Argentina | Name | Australia | Name | Canada | Name | Italy | Name | Thailand | Name | Turkey |
Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False |
Design Outcomes
Sequence: | 178566819 | Sequence: | 178566820 | Sequence: | 178566821 |
Outcome Type | primary | Outcome Type | primary | Outcome Type | primary |
Measure | Define the natural history of plasminogen deficiency | Measure | Identify factors that contribute to or correlate with disease expression and severity | Measure | Create a specimen biobank |
Time Frame | 2 years | Time Frame | 5 years | Time Frame | 15 years |
Description | Recruit 100 subjects with hypoplasminogenemia and their first-degree family members Collect up to 1 year retrospective and 3 year prospective data on symptoms, treatment and interventions |
Description | Perform centralized plasminogen activity and antigen analyses Perform centralized genetic analysis to identify changes in the plasminogen gene Perform centralized analysis of polymorphisms that affect plasminogen activity levels and impact fibrinolysis Perform local urine analysis Collect samples to explore the interaction of altered plasminogen proteins with bacterial strains |
Description | Bank plasma, serum and DNA on consenting enrolled subjects |
Sponsors
Sequence: | 48613450 | Sequence: | 48613451 |
Agency Class | OTHER | Agency Class | OTHER |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator |
Name | Indiana Hemophilia &Thrombosis Center, Inc. | Name | Fondazione Angelo Bianchi Bonomi |
Overall Officials
Sequence: | 29451026 | Sequence: | 29451027 |
Role | Principal Investigator | Role | Principal Investigator |
Name | Amy D Shapiro, MD | Name | Flora Peyvandi, MD, PhD |
Affiliation | Indiana Hemophilia &Thrombosis Center, Inc. | Affiliation | Univeristy of Milan |
Central Contacts
Sequence: | 12090738 | Sequence: | 12090739 |
Contact Type | primary | Contact Type | backup |
Name | Amy D Shapiro, MD | Name | Charles Nakar, MD |
Phone | 317-871-0000 | Phone | 317-871-0000 |
ashapiro@ihtc.org | cnakar@ihtc.org | ||
Role | Contact | Role | Contact |
Eligibilities
Sequence: | 30946771 |
Sampling Method | Probability Sample |
Gender | All |
Minimum Age | N/A |
Maximum Age | N/A |
Healthy Volunteers | No |
Population | Study population will include males and females affected with hyposplasminogenemia of any age and their first degree family members (siblings and parents). |
Criteria | Inclusion Criteria:
Signed informed consent and assent as applicable (Appendix 1) Exclusion Criteria: Previous organ transplant recipient |
Adult | True |
Child | True |
Older Adult | True |
Calculated Values
Sequence: | 254313857 |
Number Of Facilities | 15 |
Registered In Calendar Year | 2018 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | False |
Number Of Primary Outcomes To Measure | 3 |
Designs
Sequence: | 30692368 |
Observational Model | Cohort |
Time Perspective | Other |
Responsible Parties
Sequence: | 29059118 |
Responsible Party Type | Principal Investigator |
Name | Amy D Shapiro, MD |
Title | Medical Director |
Affiliation | Indiana Hemophilia &Thrombosis Center, Inc. |
Study References
Sequence: | 52396186 | Sequence: | 52396187 | Sequence: | 52396188 | Sequence: | 52396189 | Sequence: | 52396190 | Sequence: | 52396191 |
Pmid | 32001536 | Pmid | 1455395 | Pmid | 17900274 | Pmid | 25208887 | Pmid | 27629020 | Pmid | 29321155 |
Reference Type | background | Reference Type | result | Reference Type | result | Reference Type | result | Reference Type | result | Reference Type | result |
Citation | Shapiro AD, Menegatti M, Palla R, Boscarino M, Roberson C, Lanzi P, Bowen J, Nakar C, Janson IA, Peyvandi F. An international registry of patients with plasminogen deficiency (HISTORY). Haematologica. 2020 Mar;105(3):554-561. doi: 10.3324/haematol.2019.241158. Epub 2020 Jan 30. | Citation | Tait RC, Walker ID, Conkie JA, Islam SI, McCall F, Mitchell R, Davidson JF. Plasminogen levels in healthy volunteers–influence of age, sex, smoking and oral contraceptives. Thromb Haemost. 1992 Nov 10;68(5):506-10. | Citation | Schuster V, Hugle B, Tefs K. Plasminogen deficiency. J Thromb Haemost. 2007 Dec;5(12):2315-22. doi: 10.1111/j.1538-7836.2007.02776.x. Epub 2007 Sep 26. | Citation | Ma Q, Ozel AB, Ramdas S, McGee B, Khoriaty R, Siemieniak D, Li HD, Guan Y, Brody LC, Mills JL, Molloy AM, Ginsburg D, Li JZ, Desch KC. Genetic variants in PLG, LPA, and SIGLEC 14 as well as smoking contribute to plasma plasminogen levels. Blood. 2014 Nov 13;124(20):3155-64. doi: 10.1182/blood-2014-03-560086. Epub 2014 Sep 10. | Citation | Celkan T. Plasminogen deficiency. J Thromb Thrombolysis. 2017 Jan;43(1):132-138. doi: 10.1007/s11239-016-1416-6. | Citation | Shapiro AD, Nakar C, Parker JM, Albert GR, Moran JE, Thibaudeau K, Thukral N, Hardesty BM, Laurin P, Sandset PM. Plasminogen replacement therapy for the treatment of children and adults with congenital plasminogen deficiency. Blood. 2018 Mar 22;131(12):1301-1310. doi: 10.1182/blood-2017-09-806729. Epub 2018 Jan 10. |
]]>
https://zephyrnet.com/NCT03797482
2017-11-27
https://zephyrnet.com/?p=NCT03797482
NCT03797482https://www.clinicaltrials.gov/study/NCT03797482?tab=tableRohini A Hawaldarrwhawaldar@gmail.com09820432613To understand the effects induced by acute hypoxia that sets in during surgery in breast cancer. To study this, clinical samples (Tumor biopsies) will be obtained during the surgery after partial devascularisation (sample B) and stored for future genomic and proteonomic evaluations.
<![CDATA[
Studies
Study First Submitted Date | 2018-06-28 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2023-04-12 |
Start Month Year | November 27, 2017 |
Primary Completion Month Year | July 30, 2024 |
Verification Month Year | April 2023 |
Verification Date | 2023-04-30 |
Last Update Posted Date | 2023-04-12 |
Detailed Descriptions
Sequence: | 20688627 |
Description | Three tumor samples will be obtained after the patient is under anaesthesia,
Prior to starting surgery (Sample A) To understand the effects induced by acute hypoxia that sets in during surgery in breast cancer. To study this, clinical samples (Tumor biopsies) will be obtained during and stored for future genomic and proteonomic evaluations. |
Facilities
Sequence: | 199692716 |
Status | Recruiting |
Name | Tata Memorial Center |
City | Mumbai |
State | Maharashtra |
Zip | 400012 |
Country | India |
Facility Contacts
Sequence: | 28067325 | Sequence: | 28067326 |
Facility Id | 199692716 | Facility Id | 199692716 |
Contact Type | primary | Contact Type | backup |
Name | Shalaka Joshi, MS, MCh | Name | Rohini A Hawaldar, BSc |
drjoshishalaka@gmail.com | rwhawaldar@gmail.com | ||
Phone | 22241608601 | Phone | 09820432613 |
Phone Extension | 4265 |
Conditions
Sequence: | 52083075 |
Name | Breast Cancer Female |
Downcase Name | breast cancer female |
Id Information
Sequence: | 40088395 |
Id Source | org_study_id |
Id Value | Protocol 254 |
Countries
Sequence: | 42488168 |
Name | India |
Removed | False |
Design Groups
Sequence: | 55497029 |
Title | Intra-operative tumour tissue biopsies |
Description | Intra-operative tumour tissue biopsies will be collected for all patients |
Interventions
Sequence: | 52396226 |
Intervention Type | Procedure |
Name | Intra-operative Tumor Tissue Biopsy |
Description | The changing pattern of gene expression during surgery has never been studied. This could be an effect of acute hypoxia that sets in the tumour during surgery or could be a surgical response. To study these changes happening in the tumour during surgery, we are taking serial biopsies during surgery, one at the beginning, one midway during surgery and one at the end of surgery. These samples will be snap frozen and stored at -80 deg celsius in biorepository for future analysis. |
Design Outcomes
Sequence: | 177079396 | Sequence: | 177079397 |
Outcome Type | primary | Outcome Type | secondary |
Measure | Gene expression changes | Measure | Immunohistochemistry for other markers |
Time Frame | The study aims to evaluate gene expression changes during surgical resection, which lasts for 30-90 minutes on an average. Thus, we have not planned a clinical follow-up or collection of data for the patients post sampling during surgical resection. | Time Frame | The study aims to evaluate gene expression changes during surgical resection, which lasts for 30-90 minutes on an average. Thus, we have not planned a clinical follow-up or collection of data for the patients post sampling during surgical resection. |
Description | The primary outcome measured will be gene expression changes during surgical resection. Messenger ribonucleic acid (mRNA) transcripts will be quantitated and their levels evaluated during different time-points of surgical resection, using high throughput omics technologies (Next generation sequencing, nanostring ncounter, qRT-PCR array). | Description | The secondary outcome measured will be protein expression changes during surgical resection. Protein levels will be quantitated, and their levels evaluated, during different time-points of surgical resection. Transcripts found to be de-regulated or changed at different time-points of surgical resection will be evaluated using IHC at protein level. We will also use high throughput omics technologies (SILAC, ITRAQ) for characterising these changes at protein levels. |
Browse Conditions
Sequence: | 193136462 | Sequence: | 193136463 | Sequence: | 193136464 | Sequence: | 193136465 | Sequence: | 193136466 | Sequence: | 193136467 | Sequence: | 193136468 |
Mesh Term | Breast Neoplasms | Mesh Term | Hypoxia | Mesh Term | Neoplasms by Site | Mesh Term | Neoplasms | Mesh Term | Breast Diseases | Mesh Term | Skin Diseases | Mesh Term | Signs and Symptoms, Respiratory |
Downcase Mesh Term | breast neoplasms | Downcase Mesh Term | hypoxia | Downcase Mesh Term | neoplasms by site | Downcase Mesh Term | neoplasms | Downcase Mesh Term | breast diseases | Downcase Mesh Term | skin diseases | Downcase Mesh Term | signs and symptoms, respiratory |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48237694 |
Agency Class | OTHER_GOV |
Lead Or Collaborator | lead |
Name | Tata Memorial Hospital |
Overall Officials
Sequence: | 29233857 |
Role | Principal Investigator |
Name | Rajendra Badwe |
Affiliation | Director, tata Memorial Centre |
Central Contacts
Sequence: | 11990529 | Sequence: | 11990530 |
Contact Type | primary | Contact Type | backup |
Name | Shalaka Joshi, MS, MCh | Name | Rohini A Hawaldar |
Phone | 9869089803 | Phone | 09820432613 |
drjoshishalaka@gmail.com | rwhawaldar@gmail.com | ||
Phone Extension | 4265 | ||
Role | Contact | Role | Contact |
Design Group Interventions
Sequence: | 68032208 |
Design Group Id | 55497029 |
Intervention Id | 52396226 |
Eligibilities
Sequence: | 30714233 |
Sampling Method | Non-Probability Sample |
Gender | Female |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Population | Women diagnosed with breast cancer at outpatient clinic |
Criteria | Inclusion Criteria:
Clinically diagnosis of breast cancer (by FNAC or Biopsy) Exclusion Criteria: Clinically diagnosis of Metastatic breast cancer |
Gender Description | Women diagnosed with breast cancer, undergoing surgery upfront |
Gender Based | True |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253946115 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2018 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 1 |
Designs
Sequence: | 30460801 |
Observational Model | Other |
Time Perspective | Prospective |
Intervention Other Names
Sequence: | 26624003 |
Intervention Id | 52396226 |
Name | Breast cancer surgery |
Responsible Parties
Sequence: | 28827262 |
Responsible Party Type | Principal Investigator |
Name | Dr Rajendra A. Badwe |
Title | Director, Tata Memorial Centre and Professor, Department of Surgical Oncology |
Affiliation | Tata Memorial Centre |
Study References
Sequence: | 51979274 | Sequence: | 51979275 | Sequence: | 51979276 |
Pmid | 23222717 | Pmid | 11395851 | Pmid | 23915189 |
Reference Type | background | Reference Type | background | Reference Type | background |
Citation | Semenza GL. Cancer-stromal cell interactions mediated by hypoxia-inducible factors promote angiogenesis, lymphangiogenesis, and metastasis. Oncogene. 2013 Aug 29;32(35):4057-63. doi: 10.1038/onc.2012.578. Epub 2012 Dec 10. | Citation | Hockel M, Vaupel P. Biological consequences of tumor hypoxia. Semin Oncol. 2001 Apr;28(2 Suppl 8):36-41. | Citation | Hoesel B, Schmid JA. The complexity of NF-kappaB signaling in inflammation and cancer. Mol Cancer. 2013 Aug 2;12:86. doi: 10.1186/1476-4598-12-86. |
]]>
https://zephyrnet.com/NCT03797469
2019-04-15
https://zephyrnet.com/?p=NCT03797469
NCT03797469https://www.clinicaltrials.gov/study/NCT03797469?tab=tableNANANAThis study seeks to test whether these over-the-counter nutritional supplements have an impact on patients’ performance during visual field testing.
<![CDATA[
Studies
Study First Submitted Date | 2018-05-28 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2021-11-11 |
Start Month Year | April 15, 2019 |
Primary Completion Month Year | December 31, 2020 |
Verification Month Year | November 2021 |
Verification Date | 2021-11-30 |
Last Update Posted Date | 2021-11-11 |
Detailed Descriptions
Sequence: | 20795555 |
Description | Glaucoma is the leading cause of irreversible blindness worldwide. The most important test to detect progression is visual field testing. Visual field testing is the reference standard to measure visual function in glaucoma. It is called called standard automated perimetry (SAP). However, this test is very subjective, often unreliable, and variable. One of the main causes of unreliable tests is the lack of attentiveness or concentration during the test. Previous studies have shown that listening to Mozart or taking vitamin B12 can improve the reliability of this test. Recent studies have suggested that over-the-counter medications such as nicotinamide (vitamin B3) and pyruvate can also improve the performance during this test. This can ultimately reduce costs due to repeated testing and increase doctor's certainty when analyzing the results of this test. |
Facilities
Sequence: | 200759979 |
Name | Columbia University Medical Center |
City | New York |
State | New York |
Zip | 10032 |
Country | United States |
Browse Interventions
Sequence: | 96349735 | Sequence: | 96349736 | Sequence: | 96349737 | Sequence: | 96349738 | Sequence: | 96349739 | Sequence: | 96349740 | Sequence: | 96349741 | Sequence: | 96349742 | Sequence: | 96349743 | Sequence: | 96349744 | Sequence: | 96349745 | Sequence: | 96349746 |
Mesh Term | Niacinamide | Mesh Term | Niacin | Mesh Term | Nicotinic Acids | Mesh Term | Vitamins | Mesh Term | Micronutrients | Mesh Term | Physiological Effects of Drugs | Mesh Term | Vitamin B Complex | Mesh Term | Hypolipidemic Agents | Mesh Term | Antimetabolites | Mesh Term | Molecular Mechanisms of Pharmacological Action | Mesh Term | Lipid Regulating Agents | Mesh Term | Vasodilator Agents |
Downcase Mesh Term | niacinamide | Downcase Mesh Term | niacin | Downcase Mesh Term | nicotinic acids | Downcase Mesh Term | vitamins | Downcase Mesh Term | micronutrients | Downcase Mesh Term | physiological effects of drugs | Downcase Mesh Term | vitamin b complex | Downcase Mesh Term | hypolipidemic agents | Downcase Mesh Term | antimetabolites | Downcase Mesh Term | molecular mechanisms of pharmacological action | Downcase Mesh Term | lipid regulating agents | Downcase Mesh Term | vasodilator agents |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Conditions
Sequence: | 52360965 | Sequence: | 52360966 |
Name | Visual Field Defect, Peripheral | Name | Glaucoma, Open-Angle |
Downcase Name | visual field defect, peripheral | Downcase Name | glaucoma, open-angle |
Id Information
Sequence: | 40294466 |
Id Source | org_study_id |
Id Value | AAAR8208 |
Countries
Sequence: | 42717509 |
Name | United States |
Removed | False |
Design Groups
Sequence: | 55804119 | Sequence: | 55804120 |
Group Type | Active Comparator | Group Type | Placebo Comparator |
Title | Nicotinamide and Pyruvate (N&P) | Title | Placebo |
Description | This group will receive two separate sets of tablets containing 3 x 1000 mg of Vitamin B3 (nicotinamide) and 2 x 1500 mg of Pyruvate. | Description | This group will receive an equal number of tablets as the N&P group. |
Interventions
Sequence: | 52671754 | Sequence: | 52671755 | Sequence: | 52671756 |
Intervention Type | Dietary Supplement | Intervention Type | Dietary Supplement | Intervention Type | Dietary Supplement |
Name | Vitamin B3 | Name | Pyruvate | Name | Placebo |
Description | 3 tablets of 1000 mg each will be administered orally. | Description | 2 tablets of 1500 mg each will be administered orally. | Description | Tablets will look identical to the supplements and the number of tablets will equal the amount of supplements provided. |
Keywords
Sequence: | 80129277 | Sequence: | 80129278 | Sequence: | 80129279 | Sequence: | 80129280 | Sequence: | 80129281 | Sequence: | 80129282 |
Name | Perimetry | Name | Vitamins | Name | Glaucoma | Name | Supplements | Name | Vitamin B3 | Name | Nicotinamide |
Downcase Name | perimetry | Downcase Name | vitamins | Downcase Name | glaucoma | Downcase Name | supplements | Downcase Name | vitamin b3 | Downcase Name | nicotinamide |
Design Outcomes
Sequence: | 178080272 | Sequence: | 178080273 |
Outcome Type | primary | Outcome Type | secondary |
Measure | Change in 24-2 visual field test | Measure | Change in Montreal Cognitive Assessment (MoCA) scores |
Time Frame | Up to 20 weeks | Time Frame | Up to 20 weeks |
Description | Changes in 24-2 visual field results based upon point-wise and global metrics before and after intervention, and between treatment and placebo groups will be compared. | Description | Montreal Cognitive Assessment (MoCA) score before and after intervention and correlate these changes with those seen on visual field tests will be compared. The Montreal Cognitive Assessment (MoCA) is a brief 30-question test that assesses different types of cognitive abilities. Scores on the MoCA range from zero to 30, with a score of 26 and higher generally considered normal. |
Browse Conditions
Sequence: | 194208995 | Sequence: | 194208996 | Sequence: | 194208997 | Sequence: | 194208998 |
Mesh Term | Glaucoma | Mesh Term | Glaucoma, Open-Angle | Mesh Term | Ocular Hypertension | Mesh Term | Eye Diseases |
Downcase Mesh Term | glaucoma | Downcase Mesh Term | glaucoma, open-angle | Downcase Mesh Term | ocular hypertension | Downcase Mesh Term | eye diseases |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48495865 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Columbia University |
Overall Officials
Sequence: | 29385559 |
Role | Principal Investigator |
Name | Jeffrey M Liebmann, MD |
Affiliation | Columbia University |
Design Group Interventions
Sequence: | 68407797 | Sequence: | 68407798 | Sequence: | 68407799 |
Design Group Id | 55804119 | Design Group Id | 55804119 | Design Group Id | 55804120 |
Intervention Id | 52671754 | Intervention Id | 52671755 | Intervention Id | 52671756 |
Eligibilities
Sequence: | 30874786 |
Gender | All |
Minimum Age | 40 Years |
Maximum Age | 80 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
Confirmed diagnosis of primary open-angle glaucoma; Exclusion Criteria: Significant cataract or media opacity; |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254022798 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2018 |
Actual Duration | 20 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | True |
Minimum Age Num | 40 |
Maximum Age Num | 80 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 1 |
Designs
Sequence: | 30620578 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Other |
Time Perspective | |
Masking | Triple |
Subject Masked | True |
Caregiver Masked | True |
Investigator Masked | True |
Intervention Other Names
Sequence: | 26769282 | Sequence: | 26769283 |
Intervention Id | 52671754 | Intervention Id | 52671755 |
Name | B-3 Nicotinamide | Name | Calcium Pyruvate |
Responsible Parties
Sequence: | 28987109 |
Responsible Party Type | Principal Investigator |
Name | Jeffrey Liebmann |
Title | Professor of Ophthalmology |
Affiliation | Columbia University |
Study References
Sequence: | 52264794 | Sequence: | 52264795 | Sequence: | 52264796 | Sequence: | 52264797 | Sequence: | 52264798 | Sequence: | 52264799 | Sequence: | 52264800 |
Pmid | 29497468 | Pmid | 29295624 | Pmid | 28858158 | Pmid | 28538117 | Pmid | 28487632 | Pmid | 28209901 | Pmid | 34792559 |
Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | derived |
Citation | Williams PA, Harder JM, Cardozo BH, Foxworth NE, John SWM. Nicotinamide treatment robustly protects from inherited mouse glaucoma. Commun Integr Biol. 2018 Jan 19;11(1):e1356956. doi: 10.1080/19420889.2017.1356956. eCollection 2018. | Citation | Zhang M, Ying W. NAD+ Deficiency Is a Common Central Pathological Factor of a Number of Diseases and Aging: Mechanisms and Therapeutic Implications. Antioxid Redox Signal. 2019 Feb 20;30(6):890-905. doi: 10.1089/ars.2017.7445. Epub 2018 Feb 7. | Citation | Williams PA, Harder JM, John SWM. Glaucoma as a Metabolic Optic Neuropathy: Making the Case for Nicotinamide Treatment in Glaucoma. J Glaucoma. 2017 Dec;26(12):1161-1168. doi: 10.1097/IJG.0000000000000767. | Citation | Liebmann JM, Cioffi GA. Nicking Glaucoma with Nicotinamide? N Engl J Med. 2017 May 25;376(21):2079-2081. doi: 10.1056/NEJMcibr1702486. No abstract available. | Citation | Williams PA, Harder JM, Foxworth NE, Cardozo BH, Cochran KE, John SWM. Nicotinamide and WLDS Act Together to Prevent Neurodegeneration in Glaucoma. Front Neurosci. 2017 Apr 25;11:232. doi: 10.3389/fnins.2017.00232. eCollection 2017. | Citation | Williams PA, Harder JM, Foxworth NE, Cochran KE, Philip VM, Porciatti V, Smithies O, John SW. Vitamin B3 modulates mitochondrial vulnerability and prevents glaucoma in aged mice. Science. 2017 Feb 17;355(6326):756-760. doi: 10.1126/science.aal0092. | Citation | De Moraes CG, John SWM, Williams PA, Blumberg DM, Cioffi GA, Liebmann JM. Nicotinamide and Pyruvate for Neuroenhancement in Open-Angle Glaucoma: A Phase 2 Randomized Clinical Trial. JAMA Ophthalmol. 2022 Jan 1;140(1):11-18. doi: 10.1001/jamaophthalmol.2021.4576. |
]]>
https://zephyrnet.com/NCT03797456
2019-04-01
https://zephyrnet.com/?p=NCT03797456
NCT03797456https://www.clinicaltrials.gov/study/NCT03797456?tab=tableNANANAThe phase II clinical study is to investigate the safety, tolerability, efficacy and pharmacokinetics of ICP-022.
Safety, tolerability evaluation, and anti-tumor effects of ICP-022 in Chinese patients with R/R MZL will be evaluated in approximately 110 subjects. Pharmacokinetics of ICP-022 will be evaluated in approximately 20 subjects.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2022-10-12 |
Start Month Year | April 1, 2019 |
Primary Completion Month Year | December 31, 2023 |
Verification Month Year | October 2022 |
Verification Date | 2022-10-31 |
Last Update Posted Date | 2022-10-12 |
Facilities
Sequence: | 198936606 |
Name | Beijing Cancer Hospital |
City | Beijing |
State | Beijing |
Zip | 102206 |
Country | China |
Conditions
Sequence: | 51879506 |
Name | MZL |
Downcase Name | mzl |
Id Information
Sequence: | 39927542 |
Id Source | org_study_id |
Id Value | ICP-CL-00104 |
Countries
Sequence: | 42321502 |
Name | China |
Removed | False |
Design Groups
Sequence: | 55299439 |
Group Type | Experimental |
Title | ICP-022 |
Interventions
Sequence: | 52197663 |
Intervention Type | Drug |
Name | ICP-022 |
Description | ICP-022 (tablets, 50 mg) is given orally at the dose of 150 mg/day from day 1 to day 28 of each cycle for up to a total of 6 cycles or until progression. |
Design Outcomes
Sequence: | 176408966 | Sequence: | 176408967 | Sequence: | 176408968 | Sequence: | 176408969 | Sequence: | 176408970 | Sequence: | 176408971 | Sequence: | 176408972 | Sequence: | 176408973 | Sequence: | 176408974 | Sequence: | 176408975 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Overall Response Rate (ORR) | Measure | Occurrence of adverse events and serious adverse events according to NCI-CTCAE 4.03 grading criteria in Part I | Measure | Progressioin free survival (PFS) | Measure | Duration of Response (DR) | Measure | Overall survival (OS) | Measure | Area under the concentration time curve up to the time "t" (AUC(0-t)) | Measure | Maximum plasma drug concentrations (Cmax) | Measure | Time of maximum plasma drug concentrations (Tmax) | Measure | Apparent half-life for designated elimination phases (t½) | Measure | Area under the concentration time curve up to the last data point above LOQ (AUC(last)) |
Time Frame | Up to 3 years | Time Frame | Up to 3 years | Time Frame | Up to 3 years | Time Frame | Up to 3 years | Time Frame | Up to 3 years | Time Frame | up to 4 weeks | Time Frame | up to 4 weeks | Time Frame | up to 4 weeks | Time Frame | up to 4 weeks | Time Frame | up to 4 weeks |
Description | The efficacy measured by overall response rate (ORR) in Part II according to the 2014 International Working Group NHL | Description | The safety of ICP-022 measured by the occurrence of adverse events and serious adverse events according to NCI-CTCAE 4.03 grading criteria in Part I | Description | Progression free survival (PFS) is defined as the time from registration to the first occurrence of progression or relapse as assessed by the investigator, or death from any cause. PFS for patients without disease progression, relapse, or death will be censored at the time of the last tumor assessment. | Description | Duration of response as defined as the period from the first response (at least PR) to treatment until evidence of disease progression, relapse or death of any cause. Patients alive without progression and relapse will be censored at the latest tumor assessment date or the stopping date. | Description | Overall survival is defined as the period from the induction registration to death from any cause. Patients who have not died until the time of the analysis will be censored at their last contact date. | Description | Area under the concentration time curve up to the time "t" (AUC(0-t)) of ICP-022 will be measured and calculated with noncompartmental analysis using WinNonlin. | Description | Individual plasma concentrations of ICP-022 will be measured and Cmax will be calculated with noncompartmental analysis using WinNonlin. | Description | Time of maximum plasma drug concentrations (Tmax) of ICP-022 will be recorded. | Description | Apparent half-life for designated elimination phases (t½) of ICP-022 will be measured and calculated with noncompartmental analysis using WinNonlin. | Description | Area under the concentration time curve up to the last data point above LOQ (AUC(last)) of ICP-022 will be measured and calculated with noncompartmental analysis using WinNonlin. |
Browse Conditions
Sequence: | 192307384 | Sequence: | 192307383 | Sequence: | 192307385 | Sequence: | 192307386 | Sequence: | 192307387 | Sequence: | 192307388 | Sequence: | 192307389 | Sequence: | 192307390 | Sequence: | 192307391 | Sequence: | 192307392 |
Mesh Term | Lymphoma | Mesh Term | Lymphoma, B-Cell, Marginal Zone | Mesh Term | Neoplasms by Histologic Type | Mesh Term | Neoplasms | Mesh Term | Lymphoproliferative Disorders | Mesh Term | Lymphatic Diseases | Mesh Term | Immunoproliferative Disorders | Mesh Term | Immune System Diseases | Mesh Term | Lymphoma, B-Cell | Mesh Term | Lymphoma, Non-Hodgkin |
Downcase Mesh Term | lymphoma | Downcase Mesh Term | lymphoma, b-cell, marginal zone | Downcase Mesh Term | neoplasms by histologic type | Downcase Mesh Term | neoplasms | Downcase Mesh Term | lymphoproliferative disorders | Downcase Mesh Term | lymphatic diseases | Downcase Mesh Term | immunoproliferative disorders | Downcase Mesh Term | immune system diseases | Downcase Mesh Term | lymphoma, b-cell | Downcase Mesh Term | lymphoma, non-hodgkin |
Mesh Type | mesh-ancestor | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48046371 |
Agency Class | INDUSTRY |
Lead Or Collaborator | lead |
Name | Beijing InnoCare Pharma Tech Co., Ltd. |
Overall Officials
Sequence: | 29113941 |
Role | Principal Investigator |
Name | Jun Zhu, PhD |
Affiliation | Peking University Cancer Hospital & Institute |
Design Group Interventions
Sequence: | 67793235 |
Design Group Id | 55299439 |
Intervention Id | 52197663 |
Eligibilities
Sequence: | 30593151 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 75 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Men and women between 18 and 75 years old Subjects meet the following laboratory parameters: Absolute neutrophil count (ANC) ≥ 1.5×109/L Platelet count ≥ 75×109/L, independent of growth factor support within 7 days of the first dose with study drug, Hemoglobin ≥ 75 g/L; ANC ≥ 1.0×109/L, Platelet count ≥ 50×109/L, Hemoglobin ≥ 50 g/L; if bone marrow involvement Exclusion Criteria: History of other active malignancies within 5 years of study entry, unless cured without evidence of relapse or metastasis Current clinically significant cardiovascular disease including: Any class 3 or 4 cardiac disease such as arrhythmia, congestive heart failure or myocardial infarction defined by the New York Heart Association Functional Classification, or left ventricular ejection fraction (LVEF) < 50% |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253882634 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 75 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 9 |
Designs
Sequence: | 30340809 |
Allocation | N/A |
Intervention Model | Single Group Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | None (Open Label) |
Responsible Parties
Sequence: | 28717440 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797443
2019-01-01
https://zephyrnet.com/?p=NCT03797443
NCT03797443https://www.clinicaltrials.gov/study/NCT03797443?tab=tableNANANAThe purpose of this study is to see if a combination of paclitaxel protein bound (also known as nab-paclitaxel), gemcitabine, and cisplatin when given with high dose Ascorbic Acid will be safe and effective in individuals with untreated metastatic pancreatic cancer.
Vitamin C is a nutrient found in food and dietary supplements. It protects cells and also plays a key role in making collagen (which provides strength and structure to skin, bones, tissues and tendons). High-dose vitamin C may be given by intravenous (IV) infusion (through a vein into the bloodstream) or orally (taken by mouth). When taken by intravenous infusion, vitamin C can reach much higher levels in the blood than when the same amount is taken by mouth. Some human studies of high-dose IV vitamin C in patients with cancer have shown improved quality of life, as well as improvements in physical, mental, and emotional functions, symptoms of fatigue, nausea and vomiting, pain, and appetite loss. Intravenous high-dose ascorbic acid has caused very few side effects in clinical trials.
<![CDATA[
Studies
Study First Submitted Date | 2018-12-05 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-05-31 |
Start Month Year | January 1, 2019 |
Primary Completion Month Year | January 2022 |
Verification Month Year | May 2019 |
Verification Date | 2019-05-31 |
Last Update Posted Date | 2019-05-31 |
Facilities
Sequence: | 200245306 | Sequence: | 200245307 | Sequence: | 200245308 |
Name | Piedmont Cancer Institute | Name | Piedmont Cancer Institute | Name | Piedmont Cancer Institute |
City | Atlanta | City | Fayetteville | City | Newnan |
State | Georgia | State | Georgia | State | Georgia |
Zip | 30318 | Zip | 30214 | Zip | 30265 |
Country | United States | Country | United States | Country | United States |
Browse Interventions
Sequence: | 96113860 | Sequence: | 96113861 | Sequence: | 96113862 | Sequence: | 96113863 | Sequence: | 96113864 | Sequence: | 96113865 | Sequence: | 96113866 | Sequence: | 96113867 | Sequence: | 96113868 | Sequence: | 96113869 | Sequence: | 96113870 | Sequence: | 96113871 | Sequence: | 96113872 | Sequence: | 96113873 | Sequence: | 96113874 | Sequence: | 96113875 |
Mesh Term | Ascorbic Acid | Mesh Term | Paclitaxel | Mesh Term | Gemcitabine | Mesh Term | Antineoplastic Agents, Phytogenic | Mesh Term | Antineoplastic Agents | Mesh Term | Tubulin Modulators | Mesh Term | Antimitotic Agents | Mesh Term | Mitosis Modulators | Mesh Term | Molecular Mechanisms of Pharmacological Action | Mesh Term | Vitamins | Mesh Term | Micronutrients | Mesh Term | Physiological Effects of Drugs | Mesh Term | Antimetabolites, Antineoplastic | Mesh Term | Antimetabolites | Mesh Term | Antioxidants | Mesh Term | Protective Agents |
Downcase Mesh Term | ascorbic acid | Downcase Mesh Term | paclitaxel | Downcase Mesh Term | gemcitabine | Downcase Mesh Term | antineoplastic agents, phytogenic | Downcase Mesh Term | antineoplastic agents | Downcase Mesh Term | tubulin modulators | Downcase Mesh Term | antimitotic agents | Downcase Mesh Term | mitosis modulators | Downcase Mesh Term | molecular mechanisms of pharmacological action | Downcase Mesh Term | vitamins | Downcase Mesh Term | micronutrients | Downcase Mesh Term | physiological effects of drugs | Downcase Mesh Term | antimetabolites, antineoplastic | Downcase Mesh Term | antimetabolites | Downcase Mesh Term | antioxidants | Downcase Mesh Term | protective agents |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Conditions
Sequence: | 52208628 |
Name | Metastatic Pancreatic Cancer |
Downcase Name | metastatic pancreatic cancer |
Id Information
Sequence: | 40186532 |
Id Source | org_study_id |
Id Value | PAN-VITC |
Countries
Sequence: | 42600024 |
Name | United States |
Removed | False |
Design Groups
Sequence: | 55635252 |
Group Type | Experimental |
Title | AA NABPLAGEM |
Description | Ascorbic Acid Paclitaxel protein-bound cisplatin gemcitabine |
Interventions
Sequence: | 52522570 | Sequence: | 52522567 | Sequence: | 52522568 | Sequence: | 52522569 |
Intervention Type | Drug | Intervention Type | Drug | Intervention Type | Drug | Intervention Type | Drug |
Name | Gemcitabine | Name | Ascorbic Acid | Name | nab paclitaxel | Name | Cisplatin |
Description | 30 minute IV infusion on days 1 and 8 repeated every 21 days | Description | Four escalating dose levels are planned in order to determine the MTD for Phase II
The dose level for Phase II patients will be determined following completion of the Phase 1b study based on response from 3-6 patients receiving the designated dose level of ascorbic acid. |
Description | 30 minute IV infusions on days 1 and 8 repeated every 21 days, followed by Cisplatin | Description | 60minute IV infusion on days 1 and 8 repeated every 21 days followed by Gemcitabine |
Keywords
Sequence: | 79923720 | Sequence: | 79923721 | Sequence: | 79923722 | Sequence: | 79923723 | Sequence: | 79923724 | Sequence: | 79923725 | Sequence: | 79923726 | Sequence: | 79923727 |
Name | Metastatic Pancreatic Cancer | Name | Cancer | Name | Pancreatic | Name | Vitamin C | Name | Ascorbic Acid | Name | Paclitaxel Protein Bound | Name | Cisplatin | Name | Gemcitabine |
Downcase Name | metastatic pancreatic cancer | Downcase Name | cancer | Downcase Name | pancreatic | Downcase Name | vitamin c | Downcase Name | ascorbic acid | Downcase Name | paclitaxel protein bound | Downcase Name | cisplatin | Downcase Name | gemcitabine |
Design Outcomes
Sequence: | 177513231 | Sequence: | 177513232 | Sequence: | 177513233 | Sequence: | 177513234 | Sequence: | 177513235 | Sequence: | 177513236 | Sequence: | 177513237 | Sequence: | 177513238 |
Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Maximum Tolerated Dose | Measure | Disease control rate (CR+PR+SD x18 weeks) | Measure | Incidence of Treatment | Measure | Percent of patients who normalize their CA19-9 | Measure | Overall survival (OS) | Measure | Progression free | Measure | Changes in patient's self-reported quality of life | Measure | Changes in patient's self-reported pain levels |
Time Frame | approx 63 days | Time Frame | approx 63 days | Time Frame | 63 days | Time Frame | 63 days | Time Frame | 12 weeks | Time Frame | approximately 12 weeks from last study treatment ] | Time Frame | 63 days | Time Frame | 63 days |
Description | To determine the maximum tolerated dose (MTD) of high dose ascorbic acid (AA) with triple therapy of nanoparticle paclitaxel protein bound+ cisplatin + gemcitabine (NABPLAGEM) in patients with advanced stage IV metastatic pancreatic cancer | Description | To determine the preliminary efficacy (Disease control rate of CR+ PR+SD X 18 weeks) of the combination of high dose ascorbic acid (AA) at MTD with triple therapy of nanoparticle albumin- bound paclitaxel + cisplatin + gemcitabine (NABPLAGEM) in patients with advanced stage IV metastatic pancreatic cancer. | Description | Lab testing will be completed to evaluate standard of care labs for subject safety | Description | Lab testing will be completed to evaluate normalization of CA19-19 | Description | Telephone followup will be conducted every 12 weeks from the last dose of treatment to determine survival status | Description | Telephone followup will be conducted every 12 weeks from the last dose of treatment to determine status of disease progression | Description | Changes in patient's self-reported quality of life will be determined by administering the MD Anderson Symptom Inventory for Gastrointestinal Cancer (MDASI-GI) to assess the severity of multiple gastrointestinal cancer-related syymptoms and the impact of these symptoms of daily functiong. | Description | Changes in patient's self-reported pain levels will be determined by administering the Brief Pain Inventory (BPI) to assess the severity of pain and the impact of pain on daily functions. |
Browse Conditions
Sequence: | 193629117 | Sequence: | 193629118 | Sequence: | 193629119 | Sequence: | 193629120 | Sequence: | 193629121 | Sequence: | 193629122 | Sequence: | 193629123 | Sequence: | 193629124 |
Mesh Term | Pancreatic Neoplasms | Mesh Term | Digestive System Neoplasms | Mesh Term | Neoplasms by Site | Mesh Term | Neoplasms | Mesh Term | Endocrine Gland Neoplasms | Mesh Term | Digestive System Diseases | Mesh Term | Pancreatic Diseases | Mesh Term | Endocrine System Diseases |
Downcase Mesh Term | pancreatic neoplasms | Downcase Mesh Term | digestive system neoplasms | Downcase Mesh Term | neoplasms by site | Downcase Mesh Term | neoplasms | Downcase Mesh Term | endocrine gland neoplasms | Downcase Mesh Term | digestive system diseases | Downcase Mesh Term | pancreatic diseases | Downcase Mesh Term | endocrine system diseases |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48354228 | Sequence: | 48354229 | Sequence: | 48354230 | Sequence: | 48354231 | Sequence: | 48354232 | Sequence: | 48354233 |
Agency Class | OTHER | Agency Class | OTHER | Agency Class | OTHER | Agency Class | OTHER | Agency Class | OTHER | Agency Class | OTHER |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator |
Name | Piedmont Cancer Institute | Name | Cancer Research UK | Name | Stand Up To Cancer | Name | Lustgarten Foundation | Name | Destroy Pancreatic Cancer | Name | Translational Genomics Research Institute |
Design Group Interventions
Sequence: | 68199868 | Sequence: | 68199869 | Sequence: | 68199870 | Sequence: | 68199871 |
Design Group Id | 55635252 | Design Group Id | 55635252 | Design Group Id | 55635252 | Design Group Id | 55635252 |
Intervention Id | 52522567 | Intervention Id | 52522568 | Intervention Id | 52522569 | Intervention Id | 52522570 |
Eligibilities
Sequence: | 30787181 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Be willing and able to provide written informed consent/assent for the trial. Exclusion Criteria: Patients must have received no previous radiotherapy, surgery, chemotherapy or investigational therapy for the treatment of metastatic disease. Prior treatments in the adjuvant setting with gemcitabine and/or 5-FU or gemcitabine administered as a radiation sensitizer are allowed, provided at least 6 months have elapsed since completion of the last dose and no lingering toxicities are present. |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253990154 |
Number Of Facilities | 3 |
Registered In Calendar Year | 2018 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | False |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 2 |
Number Of Secondary Outcomes To Measure | 6 |
Designs
Sequence: | 30533251 |
Allocation | N/A |
Intervention Model | Single Group Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | None (Open Label) |
Intervention Model Description | Ascorbic Acid Paclitaxel Protein Bound Cisplatin Gemcitabine |
Intervention Other Names
Sequence: | 26692239 |
Intervention Id | 52522567 |
Name | Vitamin C |
Responsible Parties
Sequence: | 28899543 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797430
2019-01-02
https://zephyrnet.com/?p=NCT03797430
NCT03797430https://www.clinicaltrials.gov/study/NCT03797430?tab=tableNANANAthe aim of this study is to determine normal values for SEBT in young national or international handball women players for determining specific level for SEBT to predict risk of injury
<![CDATA[
Studies
Study First Submitted Date | 2019-01-02 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2020-07-17 |
Start Month Year | January 2, 2019 |
Primary Completion Month Year | January 2, 2020 |
Verification Month Year | July 2020 |
Verification Date | 2020-07-31 |
Last Update Posted Date | 2020-07-17 |
Conditions
Sequence: | 52256584 |
Name | Handball Players |
Downcase Name | handball players |
Id Information
Sequence: | 40220816 |
Id Source | org_study_id |
Id Value | SEBTHAND ( 29BRC18.0254) |
Keywords
Sequence: | 79989877 | Sequence: | 79989878 | Sequence: | 79989879 | Sequence: | 79989880 |
Name | hand ball | Name | evaluation | Name | risk of injury | Name | women |
Downcase Name | hand ball | Downcase Name | evaluation | Downcase Name | risk of injury | Downcase Name | women |
Design Outcomes
Sequence: | 177692173 |
Outcome Type | primary |
Measure | determination of normal values for SEBT |
Time Frame | one day |
Description | star excursion balance test : it is a functionnal test for predicting the risk of injury |
Sponsors
Sequence: | 48399114 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | University Hospital, Brest |
Overall Officials
Sequence: | 29331573 |
Role | Principal Investigator |
Name | Marc BEAUMONT, PhD |
Affiliation | CHU Brest |
Eligibilities
Sequence: | 30815001 |
Sampling Method | Probability Sample |
Gender | Female |
Minimum Age | 14 Years |
Maximum Age | 18 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Population | national or international hanball women players, aged from 14 to 18 years old |
Criteria | Inclusion Criteria:
women Exclusion Criteria: no french language |
Gender Description | handball women players |
Gender Based | True |
Adult | True |
Child | True |
Older Adult | False |
Calculated Values
Sequence: | 254076027 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Single Facility | False |
Minimum Age Num | 14 |
Maximum Age Num | 18 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Designs
Sequence: | 30560964 |
Observational Model | Cohort |
Time Perspective | Prospective |
Responsible Parties
Sequence: | 28927368 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797417
2018-09-18
https://zephyrnet.com/?p=NCT03797417
NCT03797417https://www.clinicaltrials.gov/study/NCT03797417?tab=tableQingrong Ninitina.tn@gmail.com15109230226Vitiligo is a chronic depigmenting autoimmune-associated skin disease and a growing psychological health concern because of its low quality of life. Genetics, immunology and environment triggers contribute to the pathophysiology of vitiligo. Identify and decrease the risk factors of vitiligo is very crucial for vitiligo treatment and prevention. Emerging evidence has linked gut microbiome to human autoimmune diseases. Here the investigators will analyze 10,913 metagenomes in stool samples from 100 adult vitiligo patients and gut microbiome associated metabolites in patients serum.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-05 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-09 |
Start Month Year | September 18, 2018 |
Primary Completion Month Year | June 1, 2019 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-09 |
Detailed Descriptions
Sequence: | 20741283 |
Description | Vitiligo, an autoimmune disease of the skin, is a commonly acquired chronic depigmenting disorder characterized by loss of epidermal melanocytes and progressive depigmentation clinically, affecting from 0.5% to 1% of the world population and about 1% in China Vitiligo can be a psychologically crushing associated with low quality of life, especially in colored skinned individuals. The pathoetiology of vitiligo is multifactorial and has genetic, immunological, and environmental components. Several environment-associated mechanisms have been implicated to explain melanocyte disappearance, including ultraviolet (UV) radiation exposure, repeated mechanical or thermal stress, and exposure to chemicals (especially phenols or catechols), but epidemiologic data remain limited.
Broader gut dysbioses have been identified as potential causes or contributing factors to human autoimmune diseases; however, human studies have not yet identified microbial compositional or functional triggers that are predictive of skin autoimmunity or vitiligo. Metabolites from intestinal microbiota are key determinants of host-microbe mutualism and, consequently, the health or disease of the intestinal tract. However, whether such host-microbe crosstalk influences inflammation in peripheral tissues, such as the skin, is poorly understood. The investigators will perform a metagenome association study and serum metabolomics profiling in a cohort of vitiligo Chinese individuals. |
Facilities
Sequence: | 200280928 |
Status | Recruiting |
Name | Xijing Hospital |
City | Xi'an |
State | Shaanxi |
Zip | 710032 |
Country | China |
Facility Contacts
Sequence: | 28132946 | Sequence: | 28132947 |
Facility Id | 200280928 | Facility Id | 200280928 |
Contact Type | primary | Contact Type | backup |
Name | Xijing Hospital | Name | Qingrong Ni |
nitina.tn@gmail.com | |||
Phone | 15109230226 | ||
Phone Extension | +86 |
Conditions
Sequence: | 52221812 |
Name | Gut Microbiome |
Downcase Name | gut microbiome |
Id Information
Sequence: | 40195826 |
Id Source | org_study_id |
Id Value | XJPF-LCY-V201812 |
Countries
Sequence: | 42609803 |
Name | China |
Removed | False |
Design Groups
Sequence: | 55650105 | Sequence: | 55650106 |
Title | Disease | Title | Healthy Control |
Description | patients with vitiligo | Description | healthy control |
Keywords
Sequence: | 79942133 | Sequence: | 79942134 | Sequence: | 79942135 |
Name | Gut Microbiome | Name | Vitiligo | Name | Metabolic Pathways |
Downcase Name | gut microbiome | Downcase Name | vitiligo | Downcase Name | metabolic pathways |
Design Outcomes
Sequence: | 177562358 | Sequence: | 177562359 | Sequence: | 177562360 |
Outcome Type | primary | Outcome Type | primary | Outcome Type | primary |
Measure | Gut microbiota sequencing results by analyzing metagenomes of 16s rRNA gene or microbial genes | Measure | Gut microbiota associated metabolic pathways by using metabolomics profiling of serum samples study | Measure | Vitiligo associated activity measurements like VASI assays, serum markers detection |
Time Frame | 2018.10.1–2019.3.1 | Time Frame | 2018.12.1–2019.3.1 | Time Frame | 2019.1–2019.3.1 |
Description | Fecal samples are obtained from all recruited subjects for metagenomic sequencing. The individuals have not received any antibiotic treatment for at least one month before sample collection. In the seven days before sample collection, subjects did not take any food containing probiotics such as yogurt. Each sample was either frozen immediately at -80 °C or briefly stored in personal -20 °C freezers before transport to the laboratory within 24 h. After extracting DNA from fecal samoles, gut microbiota sequencing results by using Shotgun Strategy or Meta 16s high-throughput sequencing. | Description | All serum samples will be thawed on ice and a quality control (QC) sample, made by mixing and blending equal volumes (10 μl) of each serum sample, is used to estimate a mean profile representing all the analytes encountered during analysis. The acquired MS data pretreatments included peak selection and grouping, retention time correction, second peak grouping, and isotopes and adducts annotation, will be performed as previously described56. LC-MS raw data files will be converted into mzXML format and then analyzed by the XCMS and CAMERA toolbox with R statistical language. | Description | VASI assays will be used to evaluate patients disease condition. VASI Scoring Criteria VASI=Σall body sites (hand units) × depigmentation. Serum markers like CXCL10, IL-2, and sCD25 will be detected by ELISA kits. |
Browse Conditions
Sequence: | 193679546 | Sequence: | 193679547 | Sequence: | 193679548 | Sequence: | 193679549 |
Mesh Term | Vitiligo | Mesh Term | Hypopigmentation | Mesh Term | Pigmentation Disorders | Mesh Term | Skin Diseases |
Downcase Mesh Term | vitiligo | Downcase Mesh Term | hypopigmentation | Downcase Mesh Term | pigmentation disorders | Downcase Mesh Term | skin diseases |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48366675 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Xijing Hospital |
Overall Officials
Sequence: | 29313037 |
Role | Principal Investigator |
Name | Chunying Li |
Affiliation | Study Principal Investigator |
Central Contacts
Sequence: | 12020650 |
Contact Type | primary |
Name | Qingrong Ni |
Phone | 15109230226 |
nitina.tn@gmail.com | |
Phone Extension | +86 |
Role | Contact |
Eligibilities
Sequence: | 30794871 |
Sampling Method | Probability Sample |
Gender | All |
Minimum Age | 3 Years |
Maximum Age | 65 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Population | We recruit patients who have clinically advanced vitiligo, and barely have other diseases which may disturb our study results. |
Criteria | Inclusion Criteria:
Subjects who volunteered and signed Informed Consent Form; Exclusion Criteria: Patients who had taken systemic or local treatment with vitiligo in the last month; |
Adult | True |
Child | True |
Older Adult | True |
Calculated Values
Sequence: | 254004559 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 3 |
Maximum Age Num | 65 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 3 |
Designs
Sequence: | 30540911 |
Observational Model | Case-Control |
Time Perspective | Prospective |
Responsible Parties
Sequence: | 28907231 |
Responsible Party Type | Principal Investigator |
Name | Li Chunying-1 |
Title | Vice Chief |
Affiliation | Xijing Hospital |
]]>
https://zephyrnet.com/NCT03797404
2019-04-24
https://zephyrnet.com/?p=NCT03797404
NCT03797404https://www.clinicaltrials.gov/study/NCT03797404?tab=tableNANANAChronic airway changes, such as smooth muscle hypertrophy/hyperplasia, reticular basement membrane (RBM) thickening, goblet cells hyperplasia characterize severe asthma. Chronic inflammation, and especially eosinophilia and T2 cytokines are involved in these structural changes. The aim of this prospective observational study is to assess airway changes, assessed by bronchial biopsies before treatment, then after 6 months and 12 months, induced by mepolizumab in 40 severe asthma patients who will receive the treatment as part of their standard care. Changes in RBM thickening, in airway smooth muscle (ASM) area, in the number of PGP9 sections will be assessed on bronchial biopsies after 6 months and 12 months of mepolizumab treatment. Bronchoalveolar lavage (BAL) levels of inflammatory and remodeling mediators and of extra-cellular matrix (ECM) components will be measured after 6 months and 12 months of mepolizumab treatment. Relationship between clinical response to mepolizumab and remodeling changes after 6 months and 12 months will be assessed.
<![CDATA[
Studies
Study First Submitted Date | 2018-12-06 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2023-01-20 |
Start Month Year | April 24, 2019 |
Primary Completion Month Year | June 21, 2022 |
Verification Month Year | January 2023 |
Verification Date | 2023-01-31 |
Last Update Posted Date | 2023-01-20 |
Detailed Descriptions
Sequence: | 20722444 |
Description | Scientific Rationale & Hypothesis:
Chronic airway changes, such as smooth muscle hypertrophy/hyperplasia, reticular basement membrane thickening, goblet cells hyperplasia characterize severe asthma. Chronic inflammation, and especially eosinophilia and T2 cytokines are involved in these structural changes. Increased ASM layer has been associated with eosinophilia for example, but not RBM thickening, suggesting that differential patterns of remodeling can be observed according to inflammatory patterns. Omalizumab, an anti IgE therapy, can reduce some features of airway remodeling, especially RBM and some parameters related to ASM. No data are available on potential changes in airway remodeling induced by mepolizumab. The aim of the study is to assess airway changes, assessed by bronchial biopsies, induced by mepolizumab in severe asthma patients who will receive the treatment as part of their standard care. All asthma patients refered to the asthma clinic are proposed to participate to the COBRA cohort (French national asthma cohort). Serum and DNA are collected at inclusion and every 6 months. Fiberoptic bronchoscopy (FOB) is routinely performed as part of the standard care for difficult-to-severe asthma in our centre for many years, to assess differential diagnosis and inflammatory pattern since Fractional exhaled nitric oxide (FeNO) is not routinely performed in France. BAL and 4 to 6 bronchial biopsies are performed. Study Population: Severe asthma patients, refered to Severe Asthma Centre in Bichat and Bicetre Hospitals, receiving mepolizumab according to French recommendations (eos >300mm3 in the previous year, >2 exacerbations, despite optimal step 4-5 therapy, including daily use of steroids). Study Design & Methods: General study design Prospective, observational study in one Severe Asthma Centre : Bichat Hospital (Prof C.Taillé). 40 patients will be prospectively included during a 32 months period. This study aims to assess : Changes in RBM thickening, in ASM area after 6 months and 12 months of mepolizumab treatment The following will perform at inclusion, 6 months and 12 months after initiating mepolizumab: clinical evaluation (age, BMI, atopic status, chronic rhinosinusitis, daily doses of steroids, exacerbations…) Blood test for eosinophil count and serum conservation. Study groups/arms Group 1 (prospective) : patients initiating a mepolizumab treatment. Group 2 (retrospective): to assess airway changes that can "spontaneously" occur during a 12 month-period, a retrospective "historical group" of patients included in the previous ASMATHERM study who had 2 sets of biopsies and BAL within a 6 to 12 month-interval, without exposure to mepolizumab and without change in their treatment during this interval, will be studied as a control group . Clinical data are available at inclusion and after 12 months. Biopsies are fixed in formaldehyde and processed to paraffin wax for immunohistochemical (IHC) and morphometric studies. One biopsy will be stored at -80°C for further RNAseq analyses. RBM thickening (morphometry), ASM area and the rate of ASM-proliferating cells (PCNA immuno-staining) will be measured. PGP9 staining can assess the number of nerves in the bronchial wall. The number of inflammatory cells (eosinophils, neutrophils, mast cells, T-lymphocytes evaluated respectively by MBP, elastase, tryptase, CD4 expression) and vascular sections will also be enumerated after IHC. Eosinophils localization in the airway will be described. Cytospin preparations from BAL cell pellets will be used to assess the proportion of eosinophils and neutrophils. In parallel, the levels of different pro-inflammatory and remodeling mediators will be measured in BAL aliquots concentrated x 10, by specific Elisa and Luminex assays. • Trial plan V0: screening visit V1: inclusion visit clinical evaluation V2: 6-month visit Clinical response assessment by GETE and ACT, clinical evaluation V3: 12-month visit clinical response assessment by GETE and ACT, clinical evaluation |
Facilities
Sequence: | 200113249 |
Name | Bichat hospital |
City | Paris |
Zip | 75018 |
Country | France |
Conditions
Sequence: | 52173480 |
Name | Asthma |
Downcase Name | asthma |
Id Information
Sequence: | 40160073 | Sequence: | 40160074 |
Id Source | org_study_id | Id Source | secondary_id |
Id Value | P180501J | Id Value | 2018-002591-40 |
Id Type | EudraCT Number | ||
Countries
Sequence: | 42570357 |
Name | France |
Removed | False |
Design Groups
Sequence: | 55595508 | Sequence: | 55595509 |
Title | Mepolizumab | Title | Patients w/o mepolizumab (retrospective) |
Description | Patients receiving mepolizumab | Description | Retrospective control group of patients not exposed to mepolizumab, included in the COBRA cohort and the ASMATHERM protocol, who had 2 sets of biopsies and BAL within a 6 to 12 month-interval, without change in their treatment. Clinical data for this patients are available at inclusion and after 12 months. |
Keywords
Sequence: | 79871470 | Sequence: | 79871471 | Sequence: | 79871472 | Sequence: | 79871473 |
Name | Eosinophil | Name | Bronchial biopsies | Name | Mepolizumab | Name | Severe |
Downcase Name | eosinophil | Downcase Name | bronchial biopsies | Downcase Name | mepolizumab | Downcase Name | severe |
Design Outcomes
Sequence: | 177387163 | Sequence: | 177387164 | Sequence: | 177387162 | Sequence: | 177387135 | Sequence: | 177387136 | Sequence: | 177387137 | Sequence: | 177387138 | Sequence: | 177387139 | Sequence: | 177387140 | Sequence: | 177387141 | Sequence: | 177387142 | Sequence: | 177387143 | Sequence: | 177387144 | Sequence: | 177387145 | Sequence: | 177387146 | Sequence: | 177387147 | Sequence: | 177387148 | Sequence: | 177387149 | Sequence: | 177387150 | Sequence: | 177387151 | Sequence: | 177387152 | Sequence: | 177387153 | Sequence: | 177387154 | Sequence: | 177387155 | Sequence: | 177387156 | Sequence: | 177387157 | Sequence: | 177387158 | Sequence: | 177387159 | Sequence: | 177387160 | Sequence: | 177387161 | Sequence: | 177387165 | Sequence: | 177387166 | Sequence: | 177387167 |
Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Total lung capacity (TLC) | Measure | Residual volume (RV) | Measure | Total lung capacity (TLC) | Measure | Changes in reticular basement membrane (RBM) thickening | Measure | Changes in airway smooth muscle (ASM) area | Measure | Number of proliferating muscle cells | Measure | Number of nerve endings | Measure | Number of vascular sections | Measure | Number of infiltrating inflammatory cells in the biopsies | Measure | Number of inflammatory cells in the BAL | Measure | Proportion of eosinophils expressing MBP/IL3R | Measure | Interferon-gamma concentration | Measure | IL-13 concentration | Measure | Periostin concentration | Measure | IL-17A concentration | Measure | IL-22 concentration | Measure | IL-33 concentration | Measure | Thymic Stromal Lymphopoietin (TSLP) concentration | Measure | Fibronectin concentration | Measure | Tenascin concentration | Measure | Fibulin-1 concentration | Measure | Monocyte chemoattractant protein-1 (CCL/MCP-1) concentration | Measure | EGF concentration | Measure | bFGF concentration | Measure | PDGF-BB concentration | Measure | Total score at Asthma Control Test | Measure | Global evaluation of mepolizumab benefit | Measure | Forced expiratory volume (FEV1) | Measure | Forced expiratory volume (FEV1) | Measure | Forced expiratory volume/Vital capacity (FEV1/VC) | Measure | Residual volume (RV) | Measure | Proportion of patients with pre-bronchodilator FEV1 greater than 80% | Measure | Proportion of patients with an increase from baseline in pre-bronchodilator FEV1 greater than 20% |
Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 0, 6 and 12 months | Time Frame | 6 and 12 months | Time Frame | 6 and 12 months |
Description | Measured during lung function test, pre/post salbutamol, expressed in % of predicted value. | Description | Measured during lung function test, pre/post salbutamol, expressed in ml. | Description | Measured during lung function test, pre/post salbutamol, expressed in ml. | Description | The absolute variation in RBM thickening (µm, morphometry measurement on bronchial biopsies) over 12 months is defined as the difference between month twelve and baseline (V1).
The absolute variation in RBM thickening over 6 months is defined as the difference between month six and baseline (V1). |
Description | Measured in morphometry in µm2 and expressed as a percentage of smooth muscle surface area relative to the biopsy surface.
The absolute variation in ASM area over 12 months is defined as the difference between month twelve and baseline (V1). The absolute variation in ASM area over 6 months is defined as the difference between month six and baseline (V1). |
Description | Evaluated by anti proliferating cell nuclear antigen (PCNA) antibodies, expressed as the number of positive cells per muscle surface. | Description | Evaluated by PGP9 and expressed as number of positive cells per biopsy surface in mm2 | Description | Measured with an anti-CD31 antibody, expressed in number of sections per mm2. | Description | Number of infiltrating inflammatory cells (infiltrating neutrophils, lymphocytes and eosinophils) expressed as number of positive cells per biopsy surface in mm2 | Description | Number of inflammatory cells (neutrophils, lymphocytes and eosinophils) expressed as % of total cells in the BAL | Description | Measured on bronchial biopsies, expressed as number of cells per biopsy surface in mm2 | Description | Interferon-gamma (Th1 cytokine) will be measured in BAL and serum | Description | IL-13 (Th2 cytokine) will be measured in BAL and serum | Description | Periostin (Th2 cytokine) will be measured in BAL and serum | Description | IL-17A (Th17 cytokine) will be measured in BAL and serum | Description | IL-22 (Th17 cytokine) will be measured in BAL and serum | Description | IL-33 (innate immune cytokines) will be measured in BAL and serum | Description | TSLP (innate immune cytokines) will be measured in BAL and serum | Description | Fibronectin (soluble hallmarks of ECM remodeling) will be measured in BAL and serum | Description | Tenascin (soluble hallmarks of ECM remodeling) will be measured in BAL and serum | Description | Fibulin-1 (soluble hallmarks of ECM remodeling) will be measured in BAL and serum | Description | Will be measured in BAL and serum | Description | Will be measured in BAL and serum | Description | Will be measured in BAL and serum | Description | Will be measured in BAL and serum | Description | Measured using the Asthma Control Test (ACT) scale (range: 5 to 25). ACT assesses the frequency of shortness of breath and general asthma symptoms, use of rescue medications, the effect of asthma on daily functioning, and overall self-assessment of asthma control.
5 items, with 4-week recall (on symptoms and daily functioning) The total score ranges from 5 (poor control of asthma) to 25 (complete control of asthma), with higher scores reflecting greater asthma control. An ACT score >19 indicates well-controlled asthma. |
Description | Benefit of mepolizumab will be evaluated by patient and by physician according to the physician's Global Evaluation of Treatment Effectiveness (GETE).
Patients will be considered as "responders" if classified as "excellent response" or "good response" by their physician. |
Description | Measured during lung function test, pre/post salbutamol, expressed in ml. | Description | Measured during lung function test, pre/post salbutamol, expressed in % of predicted value. | Description | Measured during lung function test, pre/post salbutamol, expressed in % | Description | Measured during lung function test, pre/post salbutamol, expressed in % of predicted value. | Description | In order to assess functional response to treatment | Description | In order to assess functional response to treatment |
Browse Conditions
Sequence: | 193495134 | Sequence: | 193495135 | Sequence: | 193495136 | Sequence: | 193495137 | Sequence: | 193495138 | Sequence: | 193495139 | Sequence: | 193495140 | Sequence: | 193495141 | Sequence: | 193495142 | Sequence: | 193495143 | Sequence: | 193495144 |
Mesh Term | Asthma | Mesh Term | Airway Remodeling | Mesh Term | Bronchial Diseases | Mesh Term | Respiratory Tract Diseases | Mesh Term | Lung Diseases, Obstructive | Mesh Term | Lung Diseases | Mesh Term | Respiratory Hypersensitivity | Mesh Term | Hypersensitivity, Immediate | Mesh Term | Hypersensitivity | Mesh Term | Immune System Diseases | Mesh Term | Pathological Conditions, Anatomical |
Downcase Mesh Term | asthma | Downcase Mesh Term | airway remodeling | Downcase Mesh Term | bronchial diseases | Downcase Mesh Term | respiratory tract diseases | Downcase Mesh Term | lung diseases, obstructive | Downcase Mesh Term | lung diseases | Downcase Mesh Term | respiratory hypersensitivity | Downcase Mesh Term | hypersensitivity, immediate | Downcase Mesh Term | hypersensitivity | Downcase Mesh Term | immune system diseases | Downcase Mesh Term | pathological conditions, anatomical |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48321189 | Sequence: | 48321190 | Sequence: | 48321191 |
Agency Class | OTHER | Agency Class | INDUSTRY | Agency Class | OTHER_GOV |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator |
Name | Assistance Publique – Hôpitaux de Paris | Name | GlaxoSmithKline | Name | Institut National de la Santé Et de la Recherche Médicale, France |
Overall Officials
Sequence: | 29286432 |
Role | Principal Investigator |
Name | Camille TAILLE, MD, PhD |
Affiliation | Assistance Publique – Hôpitaux de Paris |
Eligibilities
Sequence: | 30766568 |
Sampling Method | Non-Probability Sample |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Population | Patients with severe uncontrolled eosinophil asthma with an indication for mepolizumab according to French recommandations (eos >300mm3 in the previous year, >2 exacerbations, despite optimal step 4-5 therapy, including daily use of steroids). |
Criteria | Inclusion criteria:
adult >18 years, Exclusion criteria : pregnancy, |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253917990 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2018 |
Actual Duration | 38 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 8 |
Number Of Secondary Outcomes To Measure | 25 |
Designs
Sequence: | 30512730 |
Observational Model | Cohort |
Time Perspective | Prospective |
Responsible Parties
Sequence: | 28879029 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797391
2018-12-13
https://zephyrnet.com/?p=NCT03797391
NCT03797391https://www.clinicaltrials.gov/study/NCT03797391?tab=tableXuemei Xiexmxie@epimab.com+86-21-61043299First-in-human, Phase I/II, Multicenter, Open-Label Study of EMB-01 in Patients with Advanced/Metastatic Solid Tumors
<![CDATA[
Studies
Study First Submitted Date | 2018-12-26 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2023-05-31 |
Start Month Year | December 13, 2018 |
Primary Completion Month Year | March 14, 2025 |
Verification Month Year | May 2023 |
Verification Date | 2023-05-31 |
Last Update Posted Date | 2023-05-31 |
Detailed Descriptions
Sequence: | 20661413 |
Description | This is a first-in-human (FIH), open-label, Phase I/II study of EMB-01, a bispecific Epidermal growth factor receptor (EGFR) and c-Mesenchymal-Epithelial Transition (cMet) antibody, in patients with advanced solid tumors who have progressed on available standard therapies or for which no standard therapy exists. The study consists of two parts: Phase I (dose escalation) and Phase II (cohort expansion). The study is planning to recruit tentatively 33-66 subjects with advanced/metastatic solid tumors in phase I and approximately 42-120 subjects with EGFR mutant and/or cMET aberrated NSCLC who have progressed on or are intolerant to standard treatment(s) (including platinum-based therapy) will be enrolled at the RP2D(s) in phase II part of the study. In phase II, patients will be assigned to five groups according to their molecular status at baseline. The trial will consist of molecular pre-screening period (Phase II only), clinical screening period (-28 to -1 days), treatment cycles (each cycle is 28 days, maximum up to 2 years), and safety follow-up period (30 days after the last dose). |
Facilities
Sequence: | 199431224 | Sequence: | 199431225 | Sequence: | 199431226 | Sequence: | 199431227 | Sequence: | 199431228 |
Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting |
Name | Dana-Farber Cancer Institute | Name | Barbara Ann Karmanos Cancer Institute | Name | Gabrail Cancer Center Research | Name | Guangdong General Hospital | Name | Shanghai Chest Hosptial |
City | Boston | City | Detroit | City | Canton | City | Guangzhou | City | Shanghai |
State | Massachusetts | State | Michigan | State | Ohio | State | Guang Dong | State | Shanghai |
Zip | 02215 | Zip | 48201 | Zip | 44718 | Zip | 510080 | Zip | 200030 |
Country | United States | Country | United States | Country | United States | Country | China | Country | China |
Conditions
Sequence: | 52014308 | Sequence: | 52014309 | Sequence: | 52014310 |
Name | Neoplasms | Name | Neoplasm Metastasis | Name | Non-Small-Cell Lung Cancer |
Downcase Name | neoplasms | Downcase Name | neoplasm metastasis | Downcase Name | non-small-cell lung cancer |
Id Information
Sequence: | 40035738 |
Id Source | org_study_id |
Id Value | EMB01X101 |
Countries
Sequence: | 42431802 | Sequence: | 42431803 |
Name | United States | Name | China |
Removed | False | Removed | False |
Design Groups
Sequence: | 55420456 |
Group Type | Experimental |
Title | Dose Escalation-Part 1, Expansion-Part 2 |
Description | In part 1, escalating dose cohort, patients will receive intravenous infusions of EMB-01 weekly (QW). The duration of each treatment cycle is 28 days (4 weeks). Dose escalation will continue until the maximum tolerated dose (MTD) or recommended phase II dose (RP2D) is reached or all planned doses are administered.
In part 2, participants will receive intravenous infusion of EMB-01 at the recommended Phase II dose (RP2D) regimen(s) once weekly. The duration of each treatment cycle is 28 days (4 weeks). |
Interventions
Sequence: | 52326680 |
Intervention Type | Drug |
Name | EMB-01 |
Description | In part 1, patients will receive intravenous infusions of EMB01 weekly (QW). Dose escalation will continue until the maximum tolerated dose (MTD) or recommended phase II dose (RP2D) is reached or all planned doses are administered.
In part 2, participants will receive intravenous infusion of EMB-01 at RP2D The duration of each treatment cycle in both part 1 and part 2 is 28 days (4 weeks). Participants may continue to receive study drug until discontinuation criteria are met. |
Keywords
Sequence: | 79616780 | Sequence: | 79616781 | Sequence: | 79616782 | Sequence: | 79616783 | Sequence: | 79616784 | Sequence: | 79616785 |
Name | Human Bispecific antibody, | Name | Epidermal Growth Factor Receptor (EGFR), | Name | c-Mesenchymal-Epithelial Transition (cMet), | Name | Neoplasms, Neoplasm Metastasis, | Name | Non-Small-Cell Lung Cancer (NSCLC), First-in-human, | Name | EMB-01, Tyrosine Kinase Inhibitor (TKI) Resistant |
Downcase Name | human bispecific antibody, | Downcase Name | epidermal growth factor receptor (egfr), | Downcase Name | c-mesenchymal-epithelial transition (cmet), | Downcase Name | neoplasms, neoplasm metastasis, | Downcase Name | non-small-cell lung cancer (nsclc), first-in-human, | Downcase Name | emb-01, tyrosine kinase inhibitor (tki) resistant |
Design Outcomes
Sequence: | 176831541 | Sequence: | 176831542 | Sequence: | 176831543 | Sequence: | 176831544 | Sequence: | 176831545 | Sequence: | 176831546 | Sequence: | 176831547 | Sequence: | 176831548 | Sequence: | 176831549 | Sequence: | 176831550 | Sequence: | 176831551 | Sequence: | 176831552 | Sequence: | 176831553 | Sequence: | 176831554 | Sequence: | 176831555 |
Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | other |
Measure | Maximum tolerated dose (MTD) (phase 1 only) | Measure | Adverse Events (AEs), and Serious Adverse Events (SAEs) | Measure | Overall Response Rate (ORR) (phase 2 only) | Measure | Maximum Serum Concentration (Cmax) | Measure | Area Under the Plasma Concentration-Time Curve (AUC) | Measure | Trough Serum Concentration (Ctrough) | Measure | Elimination half-life (t1/2) | Measure | Clearance (CL) | Measure | Volume of distribution at steady state (Vss) | Measure | Accumulation Ratio (AR) | Measure | Dose Proportionality | Measure | Anti-Drug Antibodies (ADA) | Measure | Duration Of Response (DOR) | Measure | Progression-Free Survival (PFS) | Measure | Pharmacodynamic (Soluble EGFR and cMET concentration) |
Time Frame | cycle 1 (1cycle = 28 days) | Time Frame | Screening up to follow-up (30 days after the last dose) | Time Frame | From the date fo dosing until the date of first documented progression or date of death from any cause, whichever came first, assessed up to 48 months | Time Frame | Through treatment discontinuation: an average of 6 months | Time Frame | Through treatment discontinuation: an average of 6 months | Time Frame | Through treatment discontinuation: an average of 6 months | Time Frame | Through treatment discontinuation: an average of 6 months | Time Frame | Through treatment discontinuation: an average of 6 months | Time Frame | Through treatment discontinuation: an average of 6 months | Time Frame | hrough treatment discontinuation: an average of 6 months | Time Frame | Through treatment discontinuation: an average of 6 months | Time Frame | Through study completion, an average of 7 months | Time Frame | From the date fo dosing until the date of first documented progression or date of death from any cause, whichever came first, assessed up to 48 months | Time Frame | Through treatment discontinuation: an average of 6 months | Time Frame | Through treatment discontinuation: an average of 6 months |
Description | Maximum tolerated dose | Description | Adverse Events, and Serious Adverse Events | Description | Overall Response Rate | Description | Maximum Serum Concentration | Description | Area Under the Plasma Concentration-Time Curve | Description | Trough Serum Concentration | Description | Elimination half-life | Description | Clearance | Description | volume of distribution at steady state | Description | Accumulation Ratio | Description | Dose Proportionality | Description | Anti-Drug Antibodies | Description | Duration Of Response | Description | Progression-free survival | Description | Pharmacodynamic (Soluble EGFR and cMET concentration) |
Browse Conditions
Sequence: | 192864810 | Sequence: | 192864811 | Sequence: | 192864812 | Sequence: | 192864813 | Sequence: | 192864814 | Sequence: | 192864815 | Sequence: | 192864816 | Sequence: | 192864817 | Sequence: | 192864818 | Sequence: | 192864819 | Sequence: | 192864820 | Sequence: | 192864821 | Sequence: | 192864822 |
Mesh Term | Neoplasms | Mesh Term | Carcinoma, Non-Small-Cell Lung | Mesh Term | Neoplasm Metastasis | Mesh Term | Lung Neoplasms | Mesh Term | Respiratory Tract Neoplasms | Mesh Term | Thoracic Neoplasms | Mesh Term | Neoplasms by Site | Mesh Term | Lung Diseases | Mesh Term | Respiratory Tract Diseases | Mesh Term | Carcinoma, Bronchogenic | Mesh Term | Bronchial Neoplasms | Mesh Term | Neoplastic Processes | Mesh Term | Pathologic Processes |
Downcase Mesh Term | neoplasms | Downcase Mesh Term | carcinoma, non-small-cell lung | Downcase Mesh Term | neoplasm metastasis | Downcase Mesh Term | lung neoplasms | Downcase Mesh Term | respiratory tract neoplasms | Downcase Mesh Term | thoracic neoplasms | Downcase Mesh Term | neoplasms by site | Downcase Mesh Term | lung diseases | Downcase Mesh Term | respiratory tract diseases | Downcase Mesh Term | carcinoma, bronchogenic | Downcase Mesh Term | bronchial neoplasms | Downcase Mesh Term | neoplastic processes | Downcase Mesh Term | pathologic processes |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48172882 | Sequence: | 48172883 |
Agency Class | INDUSTRY | Agency Class | INDUSTRY |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator |
Name | Shanghai EpimAb Biotherapeutics Co., Ltd. | Name | Covance |
Central Contacts
Sequence: | 11973960 | Sequence: | 11973961 |
Contact Type | primary | Contact Type | backup |
Name | Xiaodong Sun, MD | Name | Xuemei Xie |
Phone | +86-21-61043299 | Phone | +86-21-61043299 |
xdsun@epimab.com | xmxie@epimab.com | ||
Role | Contact | Role | Contact |
Design Group Interventions
Sequence: | 67938917 |
Design Group Id | 55420456 |
Intervention Id | 52326680 |
Eligibilities
Sequence: | 30673422 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Molecular Pre-screening Inclusion criteria (Phase II only) The patient must sign the molecular pre-screening Inform Consent to allow for the molecular pre-screening process. All patients must have documented evidence of EGFR and/or cMet aberrations. Screening Inclusion Criteria Able to understand and willing to sign the Informed Consent Form (ICF). Histologically/cytologically confirmed advanced/metastatic solid tumors with measurable disease [Response Evaluation Criteria in Solid Tumors (RECIST) v1.1]: Phase I: advanced/metastatic solid tumors including but not limited to NSCLC, colorectal cancer, gastric cancer and liver cancer refractory to standard therapy or for which no standard therapy is available or accessible. Phase II: Advanced/metastatic NSCLC Patients have confirmed EGFR mutant and/or cMET aberration, and have progressed after standard treatment (including platinum-based therapy) or are intolerant to standard treatment. Additionally, patients with T790M mutation have received FDA/Health Authority approved therapies (if accessible) for this indication (i.e., osimertinib) and have progressed or became intolerant. A patient who has refused all currently available therapy is allowed to enroll, but must be documented in the source record. Must have adequate organ function. Regarding prior anti-tumor therapy: Must have stopped treatment at least 4 weeks or within 5 half-lives. Exclusion Criteria: Molecular Pre-screening Exclusion Criteria (Phase II only) Subject who meets any of the follow criteria can't be proceeded to clinical screening: Patients who are unwilling to sign the molecular pre-screening ICF. Screening Exclusion Criteria Life expectancy < 3 months. |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253859444 |
Number Of Facilities | 5 |
Registered In Calendar Year | 2018 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | False |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 3 |
Number Of Secondary Outcomes To Measure | 11 |
Number Of Other Outcomes To Measure | 1 |
Designs
Sequence: | 30420189 |
Allocation | N/A |
Intervention Model | Sequential Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | None (Open Label) |
Intervention Model Description | Dose escalation followed by Protocol at 100mg, 200mg, 350mg, 500mg, 700mg, 900mg, 1200mg, 1600mg, 2100mg, 2700mg and 3000mg . |
Intervention Other Names
Sequence: | 26586999 |
Intervention Id | 52326680 |
Name | FIT-013a |
Responsible Parties
Sequence: | 28786708 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797378
2019-08-09
https://zephyrnet.com/?p=NCT03797378
NCT03797378https://www.clinicaltrials.gov/study/NCT03797378?tab=tableNANANAThe purpose of this study is to test the effects of an innovative exercise program referred to as movement-2-music (M2M) on health and fitness outcomes in adults with physical/mobility disabilities. One hundred and eight participants with physical/mobility disabilities will be recruited and randomly enrolled into one of two groups: a) M2M or b) waitlist control. The primary aim of this study is to determine the effects of a 12-week M2M program on health and fitness in participants with physical/mobility disabilities who are in one of three functional mobility groups: 1) Group I – only able to exercise while sitting, 2) Group II – able to exercise sitting and standing with/without support, and 3) Group III – able to exercise one side of the body more than the other side. The second aim is to compare the observed effects of the program in this study to a previous M2M study that groups participants based on disability type. The third aim of this study is to test whether adherence (defined as attendance to the 12-week program) affects the effects of M2M in participants with physical/mobility disabilities. The potential influences of different functional mobility and disabilities of participants on how the program affects participants’ health and fitness outcomes will also be tested.
**In response to COVID-19, the 12-week M2M intervention and all assessments have been modified from being delivered in-person at Lakeshore Foundation to being delivered remotely in real-time through videoconferencing technology.**
<![CDATA[
Studies
Study First Submitted Date | 2018-11-13 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2023-05-31 |
Start Month Year | August 9, 2019 |
Primary Completion Month Year | May 25, 2023 |
Verification Month Year | May 2023 |
Verification Date | 2023-05-31 |
Last Update Posted Date | 2023-05-31 |
Detailed Descriptions
Sequence: | 20668028 |
Description | The proposed intervention efficacy trial examines a remotely-delivered, rhythmic-based movement-2-music (eM2M) intervention with 108 adults with physical/mobility disabilities who are randomized into one of two groups: a) eM2M or b) waitlist control. The primary aim is to determine the effects of a 12-week eM2M intervention on physical and psychosocial health outcomes in participants with physical/mobility disabilities who are classified into three functional mobility groups: 1) Group I – only able to exercise while sitting, 2) Group II – able to exercise sitting and standing with/without support, and 3) Group III – able to exercise one side of the body more than the other side. The secondary aim is to compare effect sizes of the physical health outcomes including cardiorespiratory fitness, muscle strength and lower extremity function obtained in the current study to a previous M2M trial that grouped participants based on disability type. The tertiary aim of this study is to explore whether adherence (defined in terms of attendance to the 12-week intervention) moderates effects of eM2M in participants with physical/mobility disabilities. The heterogeneity of treatment effect across the physical health outcomes will also be examined using functional mobility and disability groups as moderators.
Participants will complete a set of assessments at baseline and after the 12-week intervention period remotely through videoconferencing technology. They will also be asked to complete the questionnaire portion of the assessments every 6 months and the entire set of assessments every year for up to 5 years. The assessments include cardiorespiratory fitness measured using a heart rate recovery test, grip strength measured using hand-held dynamometer, lower extremity function measured using the Short Physical Performance Battery and the Timed Up and Go test as well as questionnaires that assess health-related quality of life (NIH PROMIS 10 Global Health Items, NIH PROMIS Ability to Participate in Social Roles and Activities), physical activity (Godin Leisure Time Exercise Questionnaire), exercise self-efficacy (Exercise Self-efficacy Scale), exercise goal-setting (Exercise Goal-setting Scale), outcome expectation for exercise (Multidimensional Outcomes Expectations for Exercise Scale), social support (Social Provision Scale) and barriers in physical activity (Barriers in Physical Activity Questionnaire). In addition, at the end of the 12-week intervention, participants will be interviewed about their study experience and perceived impact of eM2M on their fitness and health. |
Facilities
Sequence: | 199504795 |
Name | UAB Research Collaborative |
City | Birmingham |
State | Alabama |
Zip | 35209 |
Country | United States |
Conditions
Sequence: | 52031128 | Sequence: | 52031129 | Sequence: | 52031130 | Sequence: | 52031131 | Sequence: | 52031132 | Sequence: | 52031133 | Sequence: | 52031134 |
Name | Spinal Cord Injuries | Name | Traumatic Brain Injury | Name | Spina Bifida | Name | Cerebral Palsy | Name | Stroke | Name | Parkinson Disease | Name | Multiple Sclerosis |
Downcase Name | spinal cord injuries | Downcase Name | traumatic brain injury | Downcase Name | spina bifida | Downcase Name | cerebral palsy | Downcase Name | stroke | Downcase Name | parkinson disease | Downcase Name | multiple sclerosis |
Id Information
Sequence: | 40048716 |
Id Source | org_study_id |
Id Value | IRB-300002645 |
Countries
Sequence: | 42446383 |
Name | United States |
Removed | False |
Design Groups
Sequence: | 55439073 | Sequence: | 55439074 |
Group Type | Experimental | Group Type | No Intervention |
Title | eM2M | Title | Waitlist Control |
Description | Participants in the eM2M arm will participate in an intervention that involves three 60-minute M2M sessions per week for 12 weeks. All sessions are delivered remotely in real-time through videoconferencing technology. At the beginning and end of each session, vital signs (heart rate, blood pressure and peripheral capillary oxygen saturation) are obtained from participants. Participants rate perceived exertion, pain, and fatigue level on a log. Participants set weekly exercise goals and expectations at first session of each week. Participants also record daily activities using a provided log. | Description | Participants in the waitlist control arm are instructed to maintain their usual activities during the 12-week intervention period and are asked to record their activities on a provided log. |
Interventions
Sequence: | 52343361 |
Intervention Type | Other |
Name | eM2M |
Description | The eM2M intervention involves three 60-minute sessions per week for 12 weeks. All sessions are delivered remotely in real-time through videoconferencing technology. The intervention uses combinations of movement patterns that target range of motion, muscle strength, cardiorespiratory fitness, balance, and breathing. Each session consists of movement routines choreographed to music, and every routine can be adapted to participants' functional ability. |
Design Outcomes
Sequence: | 176894286 | Sequence: | 176894287 | Sequence: | 176894288 | Sequence: | 176894289 | Sequence: | 176894290 | Sequence: | 176894291 | Sequence: | 176894292 | Sequence: | 176894293 | Sequence: | 176894294 | Sequence: | 176894295 | Sequence: | 176894296 | Sequence: | 176894297 |
Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other | Outcome Type | other |
Measure | Change from baseline cardiorespiratory fitness at 3 months | Measure | Change from baseline muscle strength at 3 months | Measure | Change from baseline lower extremity function at 3 months | Measure | Change from baseline lower extremity function at 3 months | Measure | Change from baseline health-related quality of life at 3 months | Measure | Change from baseline social participation at 3 months | Measure | Change from baseline physical activity at 3 months | Measure | Change from baseline barriers in physical activity at 3 months | Measure | Change from baseline exercise self-efficacy at 3 months | Measure | Change from baseline exercise goal-setting at 3 months | Measure | Change from baseline outcome expectations for exercise at 3 months | Measure | Change from baseline social support at 3 months |
Time Frame | Baseline and post 12-week intervention | Time Frame | Baseline and post 12-week intervention | Time Frame | Baseline and post 12-week intervention | Time Frame | Baseline and post 12-week intervention | Time Frame | Baseline and post 12-week intervention | Time Frame | Baseline and post 12-week intervention | Time Frame | Baseline and post 12-week intervention | Time Frame | Baseline and post 12-week intervention | Time Frame | Baseline and post 12-week intervention | Time Frame | Baseline and post 12-week intervention | Time Frame | Baseline and post 12-week intervention | Time Frame | Baseline and post 12-week intervention |
Description | The cardiorespiratory fitness is measured using a heart rate recovery test | Description | Muscle strength is measured with grip strength using a hand-held dynamometer. | Description | Lower extremity function is assessed using the Short Physical Performance Battery (SPPB) | Description | Lower extremity function will be assessed using the Timed Up and Go (TUG) test. | Description | Health-related quality of life is measured using the National Institutes of Health Patient-Reported Outcomes Measurement Information System (PROMIS) Global-10 Health Items. The instrument is a 10-item measure with the response scores ranging from 1 (very severe) to 5 (none). Two summary scores, a global physical health score and a global mental health score, can be calculated from this scale, with each score ranging from 4 to 20. Higher scores indicate better health. The total raw score is translated into a T-score for each participant for analysis. | Description | Social participation is measured using the National Institutes of Health Patient-Reported Outcomes Measurement Information System (PROMIS) Ability to Participate in Social Roles and Activities. The instrument is a 8-item measure with the response scores ranging from 1 (always) to 5 (never). The lowest possible total raw score is 8 and the highest possible score is 40. Higher scores indicate better ability to participate in social roles and activities. The total raw score is translated into a T-score for each participant for analysis. | Description | Physical activity is measured using the Godin Leisure Time Exercise Questionnaire. The questionnaire contains two questions. The first question asks participants to report weekly frequencies of activities they perform at different intensities. A total weekly leisure activity is a sum of activity scores calculated by multiplying the weekly frequencies of strenuous, moderate, and light activities by 9, 5, and 3, respectively. The second question asks participants the frequency of weekly leisure-time activities performed that are long enough to work up a sweat. | Description | Barriers in physical activity will be assessed using the Barriers in Physical Activity Questionnaire. The instrument contains 43 items. Each item is responded with either no (1) or yes (2). If response is yes, a follow-up response that ranges from 1 (very small) to 5 (very large) is selected. There are 8 domains, which include personal health, attitudes/beliefs towards physical activity, friends, family, fitness center built environment, policy/programs/staff, community built environment, and safety. Each domain score is calculated by summing the item responses with its respective item weight. Higher domain scores indicate greater perceived barriers to physical activity. | Description | Exercise self-efficacy will be assessed using the Exercise Self-Efficacy Scale. The scale contains 8 items, with response options of each item ranging from 0% (not at all confident) to 100% (highly confident). All items are summed and a mean score is calculated. Higher scores indicate higher levels of self-efficacy. | Description | Exercise goal-setting will be measured using the Exercise Goal-Setting Scale. The instrument contains 10 items with response options ranging from 1 (does not describe) to 5 (describes completely). A mean score is calculated. A higher mean score indicate better goal-setting and self-monitoring for exercise. | Description | Outcome expectations for exercise will be assessed using the Multidimensional Outcome Expectations for Exercise Scale. The instrument contains 15 items, with the response options ranging from 1 (strongly disagree) to 5 (strongly agree). Three domains of outcome expectations for exercise are assessed, which include physical outcome expectations (6 items), social outcome expectations (4 items), and self-evaluative outcome expectations (5 items). Each dimension is scored by summing the item responses. Higher scores indicate higher levels of outcome expectations for exercise. | Description | Social support will be assessed using the Social Provision Scale. The instrument contains 24 items, with the response options ranging from 1 (strongly disagree) to 4 (strongly agree). A total score is calculated by summing scores from all items. A higher score indicates a greater degree of perceived support. |
Browse Conditions
Sequence: | 192930142 | Sequence: | 192930135 | Sequence: | 192930136 | Sequence: | 192930137 | Sequence: | 192930138 | Sequence: | 192930139 | Sequence: | 192930140 | Sequence: | 192930141 | Sequence: | 192930143 | Sequence: | 192930144 | Sequence: | 192930145 | Sequence: | 192930146 | Sequence: | 192930147 | Sequence: | 192930148 | Sequence: | 192930149 | Sequence: | 192930150 | Sequence: | 192930151 | Sequence: | 192930152 | Sequence: | 192930153 | Sequence: | 192930154 | Sequence: | 192930155 | Sequence: | 192930156 | Sequence: | 192930157 | Sequence: | 192930158 | Sequence: | 192930159 | Sequence: | 192930160 | Sequence: | 192930161 | Sequence: | 192930162 |
Mesh Term | Wounds and Injuries | Mesh Term | Parkinson Disease | Mesh Term | Multiple Sclerosis | Mesh Term | Brain Injuries | Mesh Term | Spinal Cord Injuries | Mesh Term | Cerebral Palsy | Mesh Term | Brain Injuries, Traumatic | Mesh Term | Spinal Dysraphism | Mesh Term | Parkinsonian Disorders | Mesh Term | Basal Ganglia Diseases | Mesh Term | Brain Diseases | Mesh Term | Central Nervous System Diseases | Mesh Term | Nervous System Diseases | Mesh Term | Movement Disorders | Mesh Term | Synucleinopathies | Mesh Term | Neurodegenerative Diseases | Mesh Term | Demyelinating Autoimmune Diseases, CNS | Mesh Term | Autoimmune Diseases of the Nervous System | Mesh Term | Demyelinating Diseases | Mesh Term | Autoimmune Diseases | Mesh Term | Immune System Diseases | Mesh Term | Craniocerebral Trauma | Mesh Term | Trauma, Nervous System | Mesh Term | Spinal Cord Diseases | Mesh Term | Brain Damage, Chronic | Mesh Term | Neural Tube Defects | Mesh Term | Nervous System Malformations | Mesh Term | Congenital Abnormalities |
Downcase Mesh Term | wounds and injuries | Downcase Mesh Term | parkinson disease | Downcase Mesh Term | multiple sclerosis | Downcase Mesh Term | brain injuries | Downcase Mesh Term | spinal cord injuries | Downcase Mesh Term | cerebral palsy | Downcase Mesh Term | brain injuries, traumatic | Downcase Mesh Term | spinal dysraphism | Downcase Mesh Term | parkinsonian disorders | Downcase Mesh Term | basal ganglia diseases | Downcase Mesh Term | brain diseases | Downcase Mesh Term | central nervous system diseases | Downcase Mesh Term | nervous system diseases | Downcase Mesh Term | movement disorders | Downcase Mesh Term | synucleinopathies | Downcase Mesh Term | neurodegenerative diseases | Downcase Mesh Term | demyelinating autoimmune diseases, cns | Downcase Mesh Term | autoimmune diseases of the nervous system | Downcase Mesh Term | demyelinating diseases | Downcase Mesh Term | autoimmune diseases | Downcase Mesh Term | immune system diseases | Downcase Mesh Term | craniocerebral trauma | Downcase Mesh Term | trauma, nervous system | Downcase Mesh Term | spinal cord diseases | Downcase Mesh Term | brain damage, chronic | Downcase Mesh Term | neural tube defects | Downcase Mesh Term | nervous system malformations | Downcase Mesh Term | congenital abnormalities |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48188563 | Sequence: | 48188564 | Sequence: | 48188565 |
Agency Class | OTHER | Agency Class | OTHER | Agency Class | UNKNOWN |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator |
Name | University of Alabama at Birmingham | Name | Lakeshore Foundation | Name | YMCA of Greater Birmingham |
Design Group Interventions
Sequence: | 67962284 |
Design Group Id | 55439073 |
Intervention Id | 52343361 |
Eligibilities
Sequence: | 30683168 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 70 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Primary diagnosis of head injury, stroke, multiple sclerosis, spinal cord injury, spina bifida, Parkinson disease, cerebral palsy by a physician Exclusion Criteria: Participate in an exercise intervention or a similar intervention in the last 6 months |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253885473 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2018 |
Actual Duration | 46 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 70 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 2 |
Number Of Secondary Outcomes To Measure | 5 |
Number Of Other Outcomes To Measure | 5 |
Designs
Sequence: | 30429896 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Other |
Time Perspective | |
Masking | Single |
Outcomes Assessor Masked | True |
Responsible Parties
Sequence: | 28796401 |
Responsible Party Type | Principal Investigator |
Name | James Rimmer |
Title | Lakeshore Foundation Endowed Chair in Health Promotion and Rehabilitation Sciences |
Affiliation | University of Alabama at Birmingham |
Study References
Sequence: | 51920421 |
Pmid | 34743701 |
Reference Type | derived |
Citation | Young HJ, Lai B, Mehta T, Thirumalai M, Wilroy J, Yates A, Kane B, Rimmer JH. The movement-to-music (M2M) study: study protocol for a randomized controlled efficacy trial examining a rhythmic teleexercise intervention for people with physical disabilities. Trials. 2021 Nov 7;22(1):779. doi: 10.1186/s13063-021-05751-2. |
Ipd Information Types
Sequence: | 3325526 | Sequence: | 3325527 |
Name | Study Protocol | Name | Statistical Analysis Plan (SAP) |
]]>
https://zephyrnet.com/NCT03797365
2019-01-10
https://zephyrnet.com/?p=NCT03797365
NCT03797365https://www.clinicaltrials.gov/study/NCT03797365?tab=tablePierre-André MAL, residentmalpierreandre@gmail.com+33659363500This trial is a pathophysiological study evaluating the impact of a cognitive therapy on the perineal neuromuscular mechanisms in women patients with urinary incontinence.
Some research works have been realized on the impact of a cognitive load test (CLT) on the neuromuscular continence urinary mechanisms. It had been demonstrated that a CLT induced an increase in the latency of voluntary perineal contraction. It had also been demonstrated that a CLT had an influence on the involuntary perineal contraction pre-activation. Most recently, the impact of a cognitive therapy on the perineal neuromuscular mechanisms on healthy participants had been evaluated. It demonstrated that a cognitive therapy inhibited the impact of the CLT on the perineal neuromuscular mechanisms.
The present project is about the evaluation of the interest of a cognitive therapy on the neuromuscular mechanisms in case of attentional test in a urinary incontinent women population. It could conduce to new therapeutic leads for the management of urinary incontinence.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-02 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-10 |
Start Month Year | January 10, 2019 |
Primary Completion Month Year | July 2019 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-10 |
Detailed Descriptions
Sequence: | 20735962 |
Description | Objectives and results expected
Cognition seems to have an effect on the physiological mechanisms of urinary continence. Urinary continence is, among others, the effect of a good coordination between detrusor's contraction and pelvic floor muscles' contraction. A cognitive disturbance involves coordination's disturbance. It has already been demonstrated that a double task rehabilitation (between cognition and perineal muscles) could annihilate the effects induced by a cognitive disturbance on the physiological neuromuscular mechanisms of the urinary incontinence. The objective of this study is to evaluate the benefit of a double task cognitive rehabilitation for the patients with urinary incontinence (UI). Current knowledge situation Pelvic floor muscles have a major incidence for the physiological urinary continence. Even if the external anal sphincter (EAS)'s muscles are not directly involved in urinary incontinence, many studies have shown they had a synergistic contraction with levator ani muscles during the voluntary and involuntary perineal contraction . Because they are easily reachable for an electromyographic (EMG) recording, many authors have registered these muscles in order to investigate the physiologic urinary continence. Amarenco et al. had shown that pelvic floor muscles' intensity of contraction in response to a cough fit was proportional to the cough intensity in an healthy volunteers population. This correlation was beyond bladder's filling. For the patients with UI, Deffieux et al. shown a loss of correlation between cough intensity and perineal contraction. Deffieux et al. also analyzed the temporal sequence of muscle activation for the EAS during a cough fit. A perineal pre contraction in an healthy volunteers population was observed. EAS's muscles EMG activation began 210 ms (median) before external intercostal (EIC) muscles. This EAS's muscles anticipation of contraction was not found in the group of patients with UI. The observation that fewer patients were activating their AES's muscles, more the modulation of EAS's muscles contraction was distorted when coughing was made. Thubert et al. observed that the perineal contraction's latency was multiplied by 4 in case of cognitive load test (CLT) in an healthy volunteers population. CLT leads to an EAS's muscles pre activation in case of coughing effort, was also observed. A lowing of 29% of AES's muscles pre activation has been demonstrated. These results suggest that cognition is involved in urinary continence's physiological mechanisms. So it seamed to be interesting to study the impact of a double task rehabilitation (cognitive and muscular) on the urinary continence's neuromuscular mechanisms in case of diversion of attention. It was a randomized trial including two groups of healthy volunteers: one group had double task rehabilitation during 15 days, the other had no rehabilitation. After 15 days rehabilitation, in the rehabilitation's group, the attention deficit's correction restored the resistive abilities of UI in case of attention hijacking. According to the last AFU's (Association Française d'Urologie – Urology French Association) and CNGOF's (Collège national des gynécologues et obstétriciens français – French Gynecologists and Obstetricians National College) recommendations, the first intention treatment of urinary incontinence is pelvi-perineal rehabilitation. Pelvi-perineal rehabilitation conducted by a therapist is multimodal with different facets: a cognitive part (education, pelvic floor realization), a behavioral part of bladder training (modification of micturition habits), a muscle building part (voluntary contractions against resistance with and without biofeedback and electrosimulation), and also a postural work part (balance and pelvis position). Perineal rehabilitation technics' heterogeneity and the lack of description of these technics let the professionals adapt their rehabilitation's protocols. The objective of this study is to compare the results of two rehabilitation's technics in urinary incontinent patients. Methodology, study population, previous studies and feasibility Study population: The population is made of voluntary incontinent women. Inclusion criteria are the followings: Major women with stress urinary incontinence or mixed urinary incontinence or urge urinary incontinence, in need to benefit from perineal rehabilitation or cognitive-behavioral rehabilitation, women able to read, understand, accept and sign the consent. Exclusion criteria are the following: pregnant women, refusal to participate, dementia and cognitive troubles (Mini Mental State score: MMS <30). Participants will be subjects to a medical statement (antecedents, age, weight, size, UDI6 (Urogenital Distress Inventory) questioner, Contilife and Wexner scores). The absence of a mental deficit will be verifies by Mini Mental Status questioner (MMS). Ethical considerations: A "CPP" (comité de protection des personnes – persons' protection comity) have been requested and obtained for this study (N° cpp17-065a/2016-A01651-50). An information letter will be delivered to the volunteers, who will be included only after the acceptation and signature of the written consent. Volunteers' randomization: Participants will be randomized in two groups (1/1) with data processing software at the first visit at the therapist practicing the perineal rehabilitation. The first group will receive "Classical" perineal rehabilitation for duration of height weeks. The second group will receive perineal rehabilitation associated with a double task cognitive therapy for a duration of height weeks. Participants will be evaluated during the consultation. Initial evaluation of volunteers: initial evaluation will consist of an interrogation able to check the participants' antecedents and characteristics, urinary incontinence symptoms (quality life score (Contilife) and severity score (International Consultation on Incontinence Questionnaire Short Form: ICIQ-SF), Urinary Handicap Measurement (MHU – Mesure du Handicap Urinaire) and also clinical examination (Pelvic Organ Prolaps Quantification: POP-Q, Ulmsten Test, levator Testing among Oxford, ureteral mobility). In a second time, the EMG analysis will be realized. It consists in the analysis of the CLT impact on the voluntary and unvoluntary perineal contraction. The CLT used is Paced Auditory Serial addition Test (PASAT). Test arrangements are the followings: The volunteer will listen to an audiotape on witch is recorded a 61 random numbers set inconstant from 1 to 9 (for example "1, 9, 4, 5…"). The volunteer patient will have to add each pair of number in order to add the number with the previous and speak verbally the response. To test the willingly perineal contraction, the volunteer will be in a sitting position with her arms on the armrests. The practitioner will position the two electrodes with self-adhesive surface from either side of the volunteer's anus regarding to the EAS muscle. These electrodes are usually used in a setting of classical evaluation with biofeedback or electro simulation. An order will be given to the volunteer in order to contract perineal muscles when she feels a stimulus on the left wrist (an electric reflex hammer regarding to the median nerve on the inside of the left wrist). The volunteer women will have to repeat the experience in two conditions: with and without the CLT. Different settings measurement will be realized: time limit for the perineal contraction reaction (RT), that is latency between stimulus and begins of AES's EMG activity increase. The other settings will be the RT max (latency between stimulus and maximum AES's EMG activity), maximum AES's EMG activity and air under the curve for the AES's EMG activity. Volunteer's perineal contraction (following coughing instruction) will also be evaluated with and without CLT. The coughing instruction will be ordered by an impulse (Reflex hammer) on the inside of the left wrist. Two more self-adhesive detection electrodes will be glued regarding the external intercostal muscles (7th right space). Principal data analyzed will be: latency between stimulus and perineal muscles (RT1) and latency between intercostal muscles and perineal muscles (RT3). The data set will be collected using a Biopac ®, Acknowledge ®. Classical perineal rehabilitation protocol Participants will benefit from two-phases perineal rehabilitation: first phase pelvic floor muscles (PFM)'s analytic rehabilitation, then a functional rehabilitation. First phase will include the PFM's awareness and voluntary contraction learning with manual, biofeedback technics and functional electro stimulation (FES). Then, therapist will propose PFM's reinforcement under the PERFECT method (Pressure, Endurance, rapid Contraction, time measurement between each contraction sequence). These exercises will call out the manual rehabilitation technics (voluntary contraction learning, pelvic anatomy), biofeedback and electro stimulation. Electro stimulation and biofeedback will necessit the use of an electrode that serves to the electromyographic measurement with and without cognitive load test. Each classical rehabilitation session will take 30 minutes with 20 minutes of active working, twice per week. About the self-training, there will be no consensus for optimal homemade exercises, neither on the number, nor on the duration. The different authors describe very different types of protocols. The self-training program will be set up as soon as the participant will be able to realize, under therapist's manual control, a voluntary analytic contraction without synergy or command reversion. Exercises' number and characteristic will be given according to the PERFECT Scheme. For the second phase, the participant will hold a micturition calendar. With the noticed elements, a behavior analyze will be summarized in order to update the favoring situations and inappropriate situations. The objective will be the learning of perineal locking and reinstatement of anticipative postural activity for stress urinary incontinence. The strategy put in place will be organized in unlearning of deleterious perineal habits and learning new behavior program. The functional training program will be made of activation of PFM's voluntary contractions during different stains of every day life; the main goal being the perineal locking set up (PFM's voluntary contraction associated with a good abdominal and perineal synergy), this locking must be systematic before and during efforts like carrying loads, trimming, coughing. During the second phase, the physiotherapist will twice weekly perform evaluations. These evaluations are similar to those in the first phase. Cognitive associated rehabilitation protocol: Added to the classic perineal muscular rehabilitation, the cognitive associated rehabilitation group randomized participants will have to execute twice a day the rehabilitation protocol. Each cognitive rehabilitation session will take three minutes. Participants will have to synergistically execute attentional tests (N-Back Test) and execute a perineal contraction during the contraction instructions. (10 randomized auditory stimuli in three minutes). The attentional tests' difficulty will be gradually increased each 15 days. N-Back Test modalities are the followings: the participant will visualize a series of random numbers. First difficulty step will be to click the dedicated button when the volunteer will see the indicated letter. The second difficulty step will be to click the dedicated button when she will see two consecutives times the same letter. The third difficulty step will be to click the dedicated button when she will see two times the same letter separated by one different letter, and so on… The data will be saved on the digital application. Methodology: Participants will consult twice per week their therapist. An intermediary clinical and EMG recording will be done in the fourth week to evaluate the evolution of symptoms and EMG's criteria, with the same arrangements as those of the first evaluation. Participants' final evaluation: During the last visit in the eighth week, participants will be evaluated with same arrangements as those of the first evaluation. Judgment criteria: About the involuntary perineal contraction study, the principal judgment criteria will be the latency between intercostal muscles contraction and perineal muscles contraction (RT3). Secondary judgment criteria will be: latency between stimulus and perineal muscles contraction (RT1) for the voluntary perineal contraction study, MHU score obtained (Mesure du Handicap Urinaire – urinary handicap score), ICIQ (International Consultation on Incontinence Questionnaire), Contilife. Statistic analysis: Descriptive data will be expressed in the form of median and interquartile gap. The Wilcoxon Test will be used to compare quantitative values before and after rehabilitation, and Student Test to compare quantitative values between "classical perineal rehabilitation" group and "perineal rehabilitation + cognitive therapy" group. According to the literature, middle RT3 is -60ms, expected difference after rehabilitation is 16,66ms and known standard deviation is 18,7ms. For an alpha risk 5% and power 80%, it is necessary to include 20 participants by group, whether total of 40 participants. |
Conditions
Sequence: | 52208565 | Sequence: | 52208566 |
Name | Urinary Incontinence, Stress | Name | Urinary Incontinence, Urge |
Downcase Name | urinary incontinence, stress | Downcase Name | urinary incontinence, urge |
Id Information
Sequence: | 40186480 |
Id Source | org_study_id |
Id Value | cpp17-065a/2016-A01651-50 |
Design Groups
Sequence: | 55635177 | Sequence: | 55635178 |
Group Type | Active Comparator | Group Type | Experimental |
Title | Classical rehabilitation | Title | Classical and cognitive associated rehabilitation |
Description | Twenty women will benefit from two-phases perineal rehabilitation: first phase pelvic floor muscles (PFM)'s analytic rehabilitation, then a functional rehabilitation. | Description | Twenty women will receive, added to the classic perineal rehabilitation, the cognitive rehabilitation and will have to execute twice a day the rehabilitation protocol. |
Interventions
Sequence: | 52522510 | Sequence: | 52522511 |
Intervention Type | Other | Intervention Type | Behavioral |
Name | Classical rehabilitation | Name | Cognitive associated rehabilitation |
Description | Participants will benefit from two-phases perineal rehabilitation:
First phase will include the PFM's awareness and voluntary contraction learning with manual, biofeedback technics and functional electro stimulation. These exercises will call out the manual rehabilitation technics, biofeedback and electro stimulation. Each classical rehabilitation session will take 30 minutes with 20 minutes of active working, twice per week. About the self-training, there will be no consensus for optimal homemade exercises. For the second phase, a behavior analyze will be summarized in order to update the favoring and inappropriate situations. The strategy put in place will be organized in unlearning of deleterious perineal habits and learning new behavior program. The main goal will be the perineal locking set up, which must be systematic before and during efforts. During this phase, the physiotherapist will twice weekly perform evaluations (similar to those in the first phase) |
Description | The cognitive associated rehabilitation group randomized participants will have to execute twice a day the rehabilitation protocol. Each cognitive rehabilitation session will take three minutes. Participants will have to synergistically execute attentional tests (N-Back Test) and execute a perineal contraction during the contraction instructions. (10 randomized auditory stimuli in three minutes). The attentional tests' difficulty will be gradually increased each 15 days. N-Back Test modalities are the followings: the participant will visualize a series of random numbers. First difficulty step will be to click the dedicated button when the volunteer will see the indicated letter. The second difficulty step will be to click the dedicated button when she will see two consecutives times the same letter. The third difficulty step will be to click the dedicated button when she will see two times the same letter separated by one different letter, and so on… |
Design Outcomes
Sequence: | 177512962 | Sequence: | 177512963 | Sequence: | 177512964 | Sequence: | 177512965 | Sequence: | 177512966 | Sequence: | 177512967 |
Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | RT3 – EMG Latency between intercostal muscles contraction and perineal muscles contraction | Measure | RT3 – EMG Latency between intercostal muscles contraction and perineal muscles | Measure | RT1 – EMG Latency between stimulus and perineal muscles contraction | Measure | Urinary Handicap Measurement (Mesure du Handicap Urinaire – MHU) | Measure | International Consultation on Incontinence Questionnaire (ICIQ-SF) | Measure | Questionnaire for assessment of quality of life related to women urinary incontinence (Contilife) |
Time Frame | Final evaluation at the eighth week follow up | Time Frame | Intermediary evaluation at the fourth week follow up | Time Frame | Intermediary evaluation at the fourth week follow up, and final evaluation at the eighth week follow up | Time Frame | Intermediary evaluation at the fourth week follow up, and final evaluation at the eighth week follow up | Time Frame | Intermediary evaluation at the fourth week follow up, and final evaluation at the eighth week follow up | Time Frame | Intermediary evaluation at the fourth week follow up, and final evaluation at the eighth week follow up |
Description | EMG Latency between intercostal muscles contraction and perineal muscles contraction | Description | EMG Latency between intercostal muscles contraction and perineal muscles contraction | Description | EMG Latency between stimulus and perineal muscles contraction | Description | Urinary Handicap Measurement is a quantitative measurement of different urinary symptoms, with 7 different questions, each response is associated to a value from 0 to 4, and with a final score from 0 (lowest score, no symptoms of urinary incontinence) to 28 (Higher score, maximum urinary incontinence symptoms). | Description | The ICIQ SF is a subjective measurement of severity of urinary loss and quality of life for those with urinary incontinence. It has 4 main items (of 6 total) ask for rating of symptoms in the past 4 weeks. The actual score takes sum score of items 3+4+5 (items 1 and 2 are demographic). The final item (6) is self diagnostic item that is unscored.
Final score is from 0 (lowest score, no symptoms of urinary incontinence), to 21 (Higher score, maximum urinary incontinence symptoms). |
Description | Auto survey of 28 questions for the quality of life related to the women with urinary incontinence. There are 6 main subjects related to quality of life, and each question has a score from 0 or 1 to 5. The final score is Final score is from 23 (lowest score, no impact of urinary incontinence on quality of life), to 140 (Higher score, maximum impact of urinary incontinence on quality of life). |
Browse Conditions
Sequence: | 193628870 | Sequence: | 193628871 | Sequence: | 193628872 | Sequence: | 193628873 | Sequence: | 193628874 | Sequence: | 193628875 | Sequence: | 193628876 | Sequence: | 193628877 | Sequence: | 193628878 | Sequence: | 193628879 | Sequence: | 193628880 | Sequence: | 193628881 | Sequence: | 193628882 | Sequence: | 193628883 | Sequence: | 193628884 |
Mesh Term | Urinary Incontinence | Mesh Term | Enuresis | Mesh Term | Urinary Incontinence, Stress | Mesh Term | Urinary Incontinence, Urge | Mesh Term | Urination Disorders | Mesh Term | Urologic Diseases | Mesh Term | Female Urogenital Diseases | Mesh Term | Female Urogenital Diseases and Pregnancy Complications | Mesh Term | Urogenital Diseases | Mesh Term | Male Urogenital Diseases | Mesh Term | Lower Urinary Tract Symptoms | Mesh Term | Urological Manifestations | Mesh Term | Behavioral Symptoms | Mesh Term | Elimination Disorders | Mesh Term | Mental Disorders |
Downcase Mesh Term | urinary incontinence | Downcase Mesh Term | enuresis | Downcase Mesh Term | urinary incontinence, stress | Downcase Mesh Term | urinary incontinence, urge | Downcase Mesh Term | urination disorders | Downcase Mesh Term | urologic diseases | Downcase Mesh Term | female urogenital diseases | Downcase Mesh Term | female urogenital diseases and pregnancy complications | Downcase Mesh Term | urogenital diseases | Downcase Mesh Term | male urogenital diseases | Downcase Mesh Term | lower urinary tract symptoms | Downcase Mesh Term | urological manifestations | Downcase Mesh Term | behavioral symptoms | Downcase Mesh Term | elimination disorders | Downcase Mesh Term | mental disorders |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48354170 | Sequence: | 48354171 |
Agency Class | OTHER | Agency Class | OTHER |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator |
Name | Pierre and Marie Curie University | Name | APHP |
Overall Officials
Sequence: | 29306234 | Sequence: | 29306235 |
Role | Principal Investigator | Role | Study Chair |
Name | Thibault THUBERT, MD | Name | Pierre-André MAL, resident |
Affiliation | CHU Hotel Dieu Nantes | Affiliation | CHU Hopital Tenon APHP |
Central Contacts
Sequence: | 12017337 | Sequence: | 12017338 |
Contact Type | primary | Contact Type | backup |
Name | Thibault THUBERT, MD | Name | Pierre-André MAL, resident |
Phone | +33647697800 | Phone | +33659363500 |
Thibault.thubert@chu-nantes.fr | malpierreandre@gmail.com | ||
Role | Contact | Role | Contact |
Design Group Interventions
Sequence: | 68199784 | Sequence: | 68199785 |
Design Group Id | 55635177 | Design Group Id | 55635178 |
Intervention Id | 52522510 | Intervention Id | 52522511 |
Eligibilities
Sequence: | 30787141 |
Gender | Female |
Minimum Age | 18 Years |
Maximum Age | 80 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Major women with stress urinary incontinence or mixed urinary incontinence or urge urinary incontinence, in need to benefit from perineal rehabilitation or cognitive-behavioral rehabilitation Exclusion Criteria: Pregnant women, |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253990097 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Single Facility | False |
Minimum Age Num | 18 |
Maximum Age Num | 80 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 2 |
Number Of Secondary Outcomes To Measure | 4 |
Designs
Sequence: | 30533211 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | None (Open Label) |
Intervention Model Description | This study is a controlled randomized single blind multicentric study on a sample of 40 women stress or mixed urinary incontinent. Participants will be randomized in two groups with a 1/1 ratio with data processing software at the first visit at the therapist practicing the perineal rehabilitation. The first group will receive "Classical" perineal rehabilitation for duration of height weeks. The second group will receive perineal rehabilitation associated to a double task cognitive therapy for duration of height weeks. Participants will be evaluated during the consultation. |
Responsible Parties
Sequence: | 28899503 |
Responsible Party Type | Principal Investigator |
Name | Thubert Thibault |
Title | Principal Investigator, Medical Doctor of Gynecology |
Affiliation | Pierre and Marie Curie University |
Study References
Sequence: | 52103548 | Sequence: | 52103549 | Sequence: | 52103550 | Sequence: | 52103551 | Sequence: | 52103552 | Sequence: | 52103553 | Sequence: | 52103554 | Sequence: | 52103555 | Sequence: | 52103556 | Sequence: | 52103557 | Sequence: | 52103558 | Sequence: | 52103559 | Sequence: | 52103560 |
Pmid | 11494188 | Pmid | 15592060 | Pmid | 17934686 | Pmid | 20236751 | Pmid | 22999088 | Pmid | 19214996 | Pmid | 10813117 | Pmid | 2265941 | Pmid | 26451967 | Pmid | 24519688 | Pmid | 27794195 | Pmid | 17905093 | Pmid | 17803192 |
Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | result | Reference Type | result | Reference Type | result | Reference Type | result | Reference Type | result |
Citation | Sapsford RR, Hodges PW. Contraction of the pelvic floor muscles during abdominal maneuvers. Arch Phys Med Rehabil. 2001 Aug;82(8):1081-8. doi: 10.1053/apmr.2001.24297. | Citation | Amarenco G, Ismael SS, Lagauche D, Raibaut P, Rene-Corail P, Wolff N, Thoumie P, Haab F. Cough anal reflex: strict relationship between intravesical pressure and pelvic floor muscle electromyographic activity during cough. Urodynamic and electrophysiological study. J Urol. 2005 Jan;173(1):149-52. doi: 10.1097/01.ju.0000147305.00443.df. | Citation | Deffieux X, Hubeaux K, Porcher R, Ismael SS, Raibaut P, Amarenco G. External intercostal muscles and external anal sphincter electromyographic activity during coughing. Int Urogynecol J Pelvic Floor Dysfunct. 2008 Apr;19(4):521-4. doi: 10.1007/s00192-007-0473-y. Epub 2007 Oct 13. | Citation | Fritel X, Fauconnier A, Bader G, Cosson M, Debodinance P, Deffieux X, Denys P, Dompeyre P, Faltin D, Fatton B, Haab F, Hermieux JF, Kerdraon J, Mares P, Mellier G, Michel-Laaengh N, Nadeau C, Robain G, de Tayrac R, Jacquetin B; French College of Gynaecologists and Obstetricians. Diagnosis and management of adult female stress urinary incontinence: guidelines for clinical practice from the French College of Gynaecologists and Obstetricians. Eur J Obstet Gynecol Reprod Biol. 2010 Jul;151(1):14-9. doi: 10.1016/j.ejogrb.2010.02.041. Epub 2010 Mar 16. | Citation | Hermieu JF, Denys P, Fritel X. [Critical review of guidelines for female urinary incontinence diagnosis and treatment]. Prog Urol. 2012 Oct;22(11):636-43. doi: 10.1016/j.purol.2012.08.004. Epub 2012 Sep 10. French. | Citation | Klovning A, Avery K, Sandvik H, Hunskaar S. Comparison of two questionnaires for assessing the severity of urinary incontinence: The ICIQ-UI SF versus the incontinence severity index. Neurourol Urodyn. 2009;28(5):411-5. doi: 10.1002/nau.20674. | Citation | Rockwood TH, Church JM, Fleshman JW, Kane RL, Mavrantonis C, Thorson AG, Wexner SD, Bliss D, Lowry AC. Fecal Incontinence Quality of Life Scale: quality of life instrument for patients with fecal incontinence. Dis Colon Rectum. 2000 Jan;43(1):9-16; discussion 16-7. doi: 10.1007/BF02237236. | Citation | Horton AM Jr, Alana S. Validation of the Mini-Mental State Examination. Int J Neurosci. 1990 Aug;53(2-4):209-12. doi: 10.3109/00207459008986604. | Citation | Thubert T, Villot A, Billecocq S, Auclair L, Amarenco G, Deffieux X. Influence of a distraction task on the involuntary reflex contraction of the pelvic floor muscles following cough. Neurourol Urodyn. 2017 Jan;36(1):160-165. doi: 10.1002/nau.22903. Epub 2015 Oct 9. | Citation | Thubert T, Deffieux X, Jousse M, Guinet-Lacoste A, Ismael SS, Amarenco G. Influence of a distraction task on pelvic floor muscle contraction. Neurourol Urodyn. 2015 Feb;34(2):139-43. doi: 10.1002/nau.22524. Epub 2014 Feb 12. | Citation | Villot A, Deffieux X, Billecocq S, Auclair L, Amarenco G, Thubert T. Influence of cognitive rehabilitation on pelvic floor muscle contraction: A randomized controlled trial. Neurourol Urodyn. 2017 Aug;36(6):1636-1644. doi: 10.1002/nau.23169. Epub 2016 Oct 29. | Citation | Deffieux X, Hubeaux K, Porcher R, Ismael SS, Raibaut P, Amarenco G. Pelvic floor muscle activity during coughing: altered pattern in women with stress urinary incontinence. Urology. 2007 Sep;70(3):443-7; discussion 447-8. doi: 10.1016/j.urology.2007.03.084. | Citation | Deffieux X, Hubeaux K, Porcher R, Ismael SS, Raibaut P, Amarenco G. Abnormal pelvic response to cough in women with stress urinary incontinence. Neurourol Urodyn. 2008;27(4):291-6. doi: 10.1002/nau.20506. |
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https://zephyrnet.com/NCT03797352
2019-01-31
https://zephyrnet.com/?p=NCT03797352
NCT03797352https://www.clinicaltrials.gov/study/NCT03797352?tab=tableAssociate Professor Reshma Merchant, MDreshmaa@nuhs.edu.sg67795555Certain clinical syndromes eg frailty, sarcopenia, dementia, depression, cognitive impairment, vision impairment, falls in older adults carry an increased risk for poor health outcomes and if identified early, can be prevented, delayed or reversible. There is evidence to suggest that exercise and dietary intervention can help delay or prevent sarcopenia, frailty and dementia. Through early screening and detection of frailty and cognitive impairment, the investigators will be able to identify participants at risk of future physical or mental decline in primary care setting and ambulatory care clinics. Those prefrail, frail but ambulant with / without cognitive impairment will be randomised to dual task exercise with/without cognitive stimulation therapy and health education. The main hypothesis is that the combination of multicomponent group exercise activities and dual task exercise is effective in reversing frailty and improving cognition.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-01 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-09 |
Start Month Year | January 2019 |
Primary Completion Month Year | May 2021 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-09 |
Detailed Descriptions
Sequence: | 20721684 |
Description | Major challenges in the Singapore healthcare landscape include a rapidly aging population, due to rising life expectancy at birth combined with declining total fertility, and an epidemiological transition in the main source of disease burden from communicable and infectious conditions to non-communicable, chronic conditions. While acute care will always remain a crucial component of healthcare delivery systems, the increased healthcare burden centered on chronic diseases and the concomitant aging population is putting increased strain on healthcare resources. Frailty is reversible and progression to dementia can be delayed. From most recent study, prevalence of pre-frailty is 37% and mild cognitive impairment about 15-20%. WHO's definition of healthy ageing is maintaining functional ability. Cognicise, a dual task exercise has shown to delay decline in cognition and there are many studies which shows aerobic exercise improves endurance. Patients seen in Geriatric, Medicine Clinic or polyclinics who are prefrail, frail but ambulant with / without cognitive impairment will be randomised to dual task exercise with/without cognitive stimulation therapy and health education. In addition, high protein diet has been shown to improve muscle protein synthesis. Therefore, the aims of the study are to assess: a) Assess the effectiveness of dual task exercise with/without cognitive stimulation therapy b) Effect of health education alone for delaying the progression to dementia and mobility decline c) Assess impact of exercise on inflammatory and bone health biomarkers eg IL, TNF, Osteocalcin, sclerostin and C telopeptide in a subgroup of older adults randomly selected. |
Conditions
Sequence: | 52171373 |
Name | Frail Elderly Syndrome |
Downcase Name | frail elderly syndrome |
Id Information
Sequence: | 40158712 |
Id Source | org_study_id |
Id Value | 2108/11 |
Design Groups
Sequence: | 55593303 | Sequence: | 55593304 |
Group Type | No Intervention | Group Type | Experimental |
Title | Control | Title | Intervention |
Description | Receive healthy ageing advice every 3 months for the duration of 12 months | Description | To participate in supervised Multicomponent exercise (combined exercise and cognitive activity) up to three times a week for 6 months and receive healthy ageing advice |
Interventions
Sequence: | 52485597 |
Intervention Type | Other |
Name | Multicomponent exercise |
Description | To identify frailty and other potential health issues, and determine if Multicomponent exercise helps at-risk elderly to have better health outcomes. |
Keywords
Sequence: | 79868738 | Sequence: | 79868739 | Sequence: | 79868740 | Sequence: | 79868741 |
Name | Bone Health | Name | Cognitive Decline | Name | Health Education | Name | Mobility Decline |
Downcase Name | bone health | Downcase Name | cognitive decline | Downcase Name | health education | Downcase Name | mobility decline |
Design Outcomes
Sequence: | 177379284 | Sequence: | 177379285 | Sequence: | 177379286 | Sequence: | 177379287 | Sequence: | 177379288 | Sequence: | 177379289 | Sequence: | 177379290 | Sequence: | 177379291 |
Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Changes in frailty status | Measure | Functional improvement | Measure | Upper extremity strength | Measure | Reduction of prevalence of depression | Measure | reduction in social isolation | Measure | Improved quality of life | Measure | Improved cognition | Measure | Improved cognition |
Time Frame | 1 year | Time Frame | 1 year | Time Frame | 1 year | Time Frame | 1 year | Time Frame | 1 year | Time Frame | 1 year | Time Frame | 1 year | Time Frame | 1 year |
Description | Changes in frailty status by 5-item FRAIL scale Scale range from 0 to 5, the higher the value, the more frail (3 or greater = frailty; 1 or 2 = prefrail) | Description | Changes in short physical performance battery (SPPB) summary score 3 subscales (range from 0 to 4 for balance, gait speed and chair stand) summed to give total score range from 0 to 12. The higher the value, the better the performance of lower extremity. | Description | Changes in handgrip strength test performance (kg) | Description | Changes in Geriatric Depression Scale (GDS) Scale range from 0 to 15, the higher the score, the greater the likelihood of depression. A score > 5 points is suggestive of depression, a score ≥ 10 points is almost always indicative of depression | Description | Changes in Lubben Social Network Scale (LSNS-6). Scale range from 0 to 30, the lower the value, the more likelihood of social isolation, A score of 12 and lower delineates "at-risk" for social isolation | Description | Changes in EuroQoL-5D (EQ5D) score 5 subscales (1 to 5): Mobility, self-care, usual activities, pain/discomfort, anxiety/depressed Each subscale assessed individually. | Description | Changes in Montreal Cognitive Assessment (MoCA), the scoring range from 0 to 30, the lower the scoring, the more likelihood of cognitive impairment. A score of 26 and higher is generally considered normal. | Description | Changes in Mini Mental State Examination (MMSE) score 5 subscales: Orientation (0 to 10), Registration (0 to 3), Attention and Calculation (0 to 5), Recall (0 to 3), Language and Praxis (0 to 9). Total scale range from 0 to 30, the higher the value, the less cognitive impairment. A score of 23 or lower is indicative of cognitive impairment. |
Sponsors
Sequence: | 48319407 | Sequence: | 48319408 |
Agency Class | OTHER | Agency Class | OTHER_GOV |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator |
Name | National University Hospital, Singapore | Name | National Medical Research Council (NMRC), Singapore |
Overall Officials
Sequence: | 29285416 |
Role | Principal Investigator |
Name | Associate Professor Reshma Merchant, MD |
Affiliation | National University Hospital, Singapore |
Central Contacts
Sequence: | 12008912 |
Contact Type | primary |
Name | Associate Professor Reshma Merchant, MD |
Phone | 67795555 |
reshmaa@nuhs.edu.sg | |
Role | Contact |
Design Group Interventions
Sequence: | 68149275 |
Design Group Id | 55593304 |
Intervention Id | 52485597 |
Eligibilities
Sequence: | 30765421 |
Gender | All |
Minimum Age | 65 Years |
Maximum Age | 120 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
Pre frail or frail but ambulant (Frail scale score of at least 1) Exclusion Criteria: Unable to give consent personally |
Adult | False |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253889357 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Single Facility | False |
Minimum Age Num | 65 |
Maximum Age Num | 120 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 2 |
Number Of Secondary Outcomes To Measure | 6 |
Designs
Sequence: | 30511587 |
Allocation | Randomized |
Intervention Model | Factorial Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Single |
Investigator Masked | True |
Responsible Parties
Sequence: | 28877882 |
Responsible Party Type | Principal Investigator |
Name | Medicine |
Title | Head & Senior Consultant, Division of Geriatric Medicine |
Affiliation | National University Hospital, Singapore |
]]>
https://zephyrnet.com/NCT03797339
2017-07-01
https://zephyrnet.com/?p=NCT03797339
NCT03797339https://www.clinicaltrials.gov/study/NCT03797339?tab=tableJuer Liu, masterliujesysu@163.com13430267895This study aimed to explore underlying mechanisms of individual differences in drugs for coronary heart disease treatment and its association with adverse consequences. It will enroll approximately 4000 coronal heart disease patients aged between 18 and 80 years in mainland China and follow-up for at least 1 years. Questionnaires, anthropometric measures, laboratory tests, and biomaterials will be collected . The principal clinical outcomes of the study consist of ischemia attack , cardiac death, renal injury,and myotoxic activity.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-05 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-02-12 |
Start Month Year | July 1, 2017 |
Primary Completion Month Year | December 31, 2019 |
Verification Month Year | February 2019 |
Verification Date | 2019-02-28 |
Last Update Posted Date | 2019-02-12 |
Detailed Descriptions
Sequence: | 20741285 |
Description | The study is a multicenter prospective cohort study, aimed to explore underlying mechanisms of individual differences in drugs for coronary heart disease treatment and its association with adverse consequences.The genomic genotype, DNA methylation and metabolome of 1000 patients with coronary heart disease were determined using illumina high-density genotyping chip, high-throughput sequencing and high-resolution mass spectrometry. Blood exposures of statins and metoprolol and its metabolites was determined by UPLC-MS/MS.
The biological network using cross-omics analysis was reconstructed to identify potential causative key genes, bacteria, and endogenous metabolite targets that cause differences in individual responses. A machine identification algorithm selecting clinical factors and multi-omics targets was used to establish a predictive mathematical model. A multi-center clinical cohort of 3000 coronal heart disease patients was used to verify the effects of various levels of omic targets on drug blood exposures, efficacy and toxic side effects. A comprehensive model based on multi-target combination of individualized drugs was constructed, and the predictive effect was clinically analyzed. |
Facilities
Sequence: | 200280929 | Sequence: | 200280930 | Sequence: | 200280931 | Sequence: | 200280932 | Sequence: | 200280933 |
Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting | Status | Recruiting |
Name | Guangdong General Hospital | Name | The First Affiliated Hospital of Sun Yat-sen University | Name | XiangYa Hospital Central South University | Name | Renji Hospital Affiliated to Shanghai Jiaotong University | Name | West China Hospital, Sichuan University |
City | Guangzhou | City | Guangzhou | City | Changsha | City | Shanghai | City | Chengdu |
State | Guangdong | State | Guangdong | State | Hunan | State | Shanghai | State | Sichuan |
Zip | 510080 | Zip | 510080 | Zip | 410008 | Zip | 200233 | Zip | 610041 |
Country | China | Country | China | Country | China | Country | China | Country | China |
Facility Contacts
Sequence: | 28132948 | Sequence: | 28132949 | Sequence: | 28132950 | Sequence: | 28132951 | Sequence: | 28132952 |
Facility Id | 200280929 | Facility Id | 200280930 | Facility Id | 200280931 | Facility Id | 200280932 | Facility Id | 200280933 |
Contact Type | primary | Contact Type | primary | Contact Type | primary | Contact Type | primary | Contact Type | primary |
Name | Shilong Zhong, Ph.D | Name | Chen Liu, MD, PhD | Name | Qilin Ma, MD | Name | Linghong Shen, MD, PhD | Name | Liang Ouyang, PhD |
zhongsl@hotmail.com | chenliu81@hotmail.com | mqilin2004@163.com | drshenlinghong@126.com | ouyangliang@scu.edu.cn | |||||
Phone | 8618620819696 | Phone | 8615013270269 | Phone | 86731-84327203 | Phone | 8613916495713 | Phone | 8613880674611 |
Conditions
Sequence: | 52221814 |
Name | Coronary Heart Disease |
Downcase Name | coronary heart disease |
Id Information
Sequence: | 40195828 |
Id Source | org_study_id |
Id Value | 2017YFC0909301 |
Countries
Sequence: | 42609804 |
Name | China |
Removed | False |
Design Groups
Sequence: | 55650109 | Sequence: | 55650110 |
Title | Discovery cohort | Title | Validation corhort |
Description | 1000 cases of coronary heart disease follow-up cohort was used for multi-omics target discovery.During the follow-up period, the information about the occurrence and risk factors of adverse cardiovascular events will be collected. | Description | 3000 coronary heart disease follow-up cohorts was used for validating the results from the discovery corhort. During the follow-up period, the occurrence and risk factors of adverse cardiovascular events.Predictive mathematical models based on multi-omics combination will be constructed finally. |
Interventions
Sequence: | 52535611 | Sequence: | 52535612 | Sequence: | 52535613 | Sequence: | 52535614 |
Intervention Type | Other | Intervention Type | Other | Intervention Type | Other | Intervention Type | Other |
Name | risk factors of adverse cardiovascular events | Name | multi-omics target discovery | Name | validation | Name | Predictive mathematical models |
Description | During the follow-up period,general information(age, sex, BMI, blood pressure, the history of drink and smoke, medical history, etc).Blood biochemistry parameters(Lipid, hsCRP levels, etc)and other laboratory examination parameters will be collected | Description | Genome-wide genotype , DNA methylation and metabolomes were determined using illumina high-density genotyping chips, high-throughput sequencing, and high-resolution mass spectrometry respectly. Blood exposure of statins and metoprolol and its metabolites was determined by UPLC-MS/MS. | Description | The genome-wide genotype of patients with coronary heart disease was detected using the illumina chip. The methylation level of the functional region was detected by the target region enrichment methylation sequencing method. Intestinal flora differences were detected using 16SrDNA high-throughput sequencing. | Description | Machine learning algorithms such as multiple linear regression or Bayesian classification are used to optimize clinical factors and multi-group targets to establish predictive mathematical models. |
Keywords
Sequence: | 79942136 | Sequence: | 79942137 | Sequence: | 79942138 | Sequence: | 79942139 | Sequence: | 79942140 | Sequence: | 79942141 |
Name | epigenome | Name | metabolome | Name | microbiome | Name | genome | Name | multi-omics targets | Name | individual drug use |
Downcase Name | epigenome | Downcase Name | metabolome | Downcase Name | microbiome | Downcase Name | genome | Downcase Name | multi-omics targets | Downcase Name | individual drug use |
Design Outcomes
Sequence: | 177562364 | Sequence: | 177562365 | Sequence: | 177562366 | Sequence: | 177562367 | Sequence: | 177562368 | Sequence: | 177562369 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | other |
Measure | Death | Measure | MACE | Measure | Bleeding | Measure | Statin-induced myopathy (SIM) | Measure | CI-AKI | Measure | SYNTAX score |
Time Frame | from date of baseline examination until the date of first documented death,up to 48 months | Time Frame | from date of baseline examination until the date of first documented cardiovascular events,up to 48 months | Time Frame | from date of baseline examination until the date of first documented bleeding,up to 48 months | Time Frame | from date of baseline examination until the date of first documented SIM,up to 48 months | Time Frame | more than 6 h within 48 h after Coronary Angiography | Time Frame | more than 6 h within 48 h after Coronary Angiography |
Description | All-cause death | Description | MACE was defined as the occurrence of cardiac death, nonfatal myocardial infarctions, coronary revascularisation and cerebral infraction. | Description | Bleeding was the six-month incidence of combined alarming, internal, and nuisance bleeding events defined according to Serebruany et al15. Alarming bleeding included bleeding requiring a transfusion, intracranial bleeding, and life-threatening bleeding. Internal bleeding included haematoma, epistaxis, blood loss from the mouth, vagina, melaena, eye bleed, haematuria, and haematemesis. Nuisance bleeding included easy bruising, bleeding from small cuts, petechiae, and ecchymosis. | Description | The definition of SIM from statin treatment was based on the patients' subjective sense of muscular pain as well as CK elevations. These muscular side effects included myalgia (muscle pain/ache without serum CK elevations), other muscle-related symptoms such as weakness, cramps, spasms, soreness and twitching, CK elevations without physical symptoms, myositis or other muscle symptoms with CK elevations, and rhabdomyolysis. | Description | CI-AKI was diagnosed if a patient had an absolute increase in serum creatinine (sCr) concentration ≥ 0.3 mg/dl (26.4 μmol/L) from baseline or a relative increase ≥ 50 % in sCr concentration for more than 6 h within 48 h after surgery | Description | It is mainly used for the treatment of left main coronary artery lesions and/or three-vessel lesions.Patients with a score of ≥33 are recommended for CABG. Patients with a score between 23 and 32 can choose either PCI or CABG. Patients with a score of ≤22 are recommended for PCI and CABG. |
Browse Conditions
Sequence: | 193679558 | Sequence: | 193679559 | Sequence: | 193679560 | Sequence: | 193679561 | Sequence: | 193679562 | Sequence: | 193679563 | Sequence: | 193679564 | Sequence: | 193679565 |
Mesh Term | Heart Diseases | Mesh Term | Coronary Disease | Mesh Term | Coronary Artery Disease | Mesh Term | Myocardial Ischemia | Mesh Term | Cardiovascular Diseases | Mesh Term | Vascular Diseases | Mesh Term | Arteriosclerosis | Mesh Term | Arterial Occlusive Diseases |
Downcase Mesh Term | heart diseases | Downcase Mesh Term | coronary disease | Downcase Mesh Term | coronary artery disease | Downcase Mesh Term | myocardial ischemia | Downcase Mesh Term | cardiovascular diseases | Downcase Mesh Term | vascular diseases | Downcase Mesh Term | arteriosclerosis | Downcase Mesh Term | arterial occlusive diseases |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48366677 | Sequence: | 48366678 | Sequence: | 48366679 | Sequence: | 48366680 | Sequence: | 48366681 |
Agency Class | OTHER | Agency Class | OTHER | Agency Class | OTHER | Agency Class | OTHER | Agency Class | OTHER |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator |
Name | Guangdong Provincial People's Hospital | Name | RenJi Hospital | Name | West China Hospital | Name | Xiangya Hospital of Central South University | Name | First Affiliated Hospital, Sun Yat-Sen University |
Overall Officials
Sequence: | 29313039 |
Role | Principal Investigator |
Name | Shilong Zhong, Ph.D |
Affiliation | Guangdong Provincial People's Hospital |
Central Contacts
Sequence: | 12020651 | Sequence: | 12020652 |
Contact Type | primary | Contact Type | backup |
Name | Shilong Zhong, Ph.D | Name | Juer Liu, master |
Phone | 862083827812 | Phone | 13430267895 |
zhongsl@hotmail.com | liujesysu@163.com | ||
Phone Extension | 51157 | Phone Extension | 51157 |
Role | Contact | Role | Contact |
Design Group Interventions
Sequence: | 68217754 | Sequence: | 68217755 | Sequence: | 68217756 | Sequence: | 68217757 | Sequence: | 68217758 |
Design Group Id | 55650109 | Design Group Id | 55650110 | Design Group Id | 55650109 | Design Group Id | 55650110 | Design Group Id | 55650110 |
Intervention Id | 52535611 | Intervention Id | 52535611 | Intervention Id | 52535612 | Intervention Id | 52535613 | Intervention Id | 52535614 |
Eligibilities
Sequence: | 30794873 |
Sampling Method | Non-Probability Sample |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 80 Years |
Healthy Volunteers | No |
Population | Chinese Han patients with coronary artery disease who have ingested metoprolol and statins were prospectively recruited from Guangdong General Hospital, Shanghai Jiao Tong University, Central South University, Sun Yat-sen University and Sichuan University. |
Criteria | Inclusion Criteria:
age: 18-80 years Exclusion Criteria: renal insufficiency (defined as serum creatinine concentration > 2 times the upper limit of normal [230 μmol/L], renal transplantation or dialysis) |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254004561 |
Number Of Facilities | 5 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | False |
Minimum Age Num | 18 |
Maximum Age Num | 80 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 4 |
Number Of Other Outcomes To Measure | 1 |
Designs
Sequence: | 30540913 |
Observational Model | Cohort |
Time Perspective | Prospective |
Responsible Parties
Sequence: | 28907233 |
Responsible Party Type | Principal Investigator |
Name | ShiLong Zhong |
Title | Professor |
Affiliation | Guangdong Provincial People's Hospital |
]]>
https://zephyrnet.com/NCT03797326
2019-02-12
https://zephyrnet.com/?p=NCT03797326
NCT03797326https://www.clinicaltrials.gov/study/NCT03797326?tab=tableNANANAThe purpose of this study is to determine the safety and efficacy of combination therapy with pembrolizumab (MK-3475) and lenvatinib (E7080/MK-7902) in participants with triple negative breast cancer (TNBC), ovarian cancer, gastric cancer, colorectal cancer (CRC), glioblastoma (GBM), biliary tract cancers (BTC), or pancreatic cancer.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2022-08-22 |
Start Month Year | February 12, 2019 |
Primary Completion Month Year | December 22, 2023 |
Verification Month Year | August 2022 |
Verification Date | 2022-08-31 |
Last Update Posted Date | 2022-08-22 |
Facilities
Sequence: | 201025693 | Sequence: | 201025694 | Sequence: | 201025695 | Sequence: | 201025696 | Sequence: | 201025697 | Sequence: | 201025698 | Sequence: | 201025699 | Sequence: | 201025700 | Sequence: | 201025701 | Sequence: | 201025702 | Sequence: | 201025703 | Sequence: | 201025704 | Sequence: | 201025705 | Sequence: | 201025706 | Sequence: | 201025707 | Sequence: | 201025708 | Sequence: | 201025709 | Sequence: | 201025710 | Sequence: | 201025711 | Sequence: | 201025712 | Sequence: | 201025713 | Sequence: | 201025714 | Sequence: | 201025715 | Sequence: | 201025716 | Sequence: | 201025717 | Sequence: | 201025718 | Sequence: | 201025719 | Sequence: | 201025720 | Sequence: | 201025721 | Sequence: | 201025722 | Sequence: | 201025723 | Sequence: | 201025724 | Sequence: | 201025725 | Sequence: | 201025726 | Sequence: | 201025727 | Sequence: | 201025728 | Sequence: | 201025729 | Sequence: | 201025730 | Sequence: | 201025731 | Sequence: | 201025732 | Sequence: | 201025733 | Sequence: | 201025734 | Sequence: | 201025735 | Sequence: | 201025736 | Sequence: | 201025737 | Sequence: | 201025738 | Sequence: | 201025739 | Sequence: | 201025740 | Sequence: | 201025741 | Sequence: | 201025742 | Sequence: | 201025743 | Sequence: | 201025744 | Sequence: | 201025745 | Sequence: | 201025746 | Sequence: | 201025747 | Sequence: | 201025748 | Sequence: | 201025749 | Sequence: | 201025750 | Sequence: | 201025751 | Sequence: | 201025752 | Sequence: | 201025753 | Sequence: | 201025754 | Sequence: | 201025755 | Sequence: | 201025756 | Sequence: | 201025757 | Sequence: | 201025758 | Sequence: | 201025759 | Sequence: | 201025760 | Sequence: | 201025761 | Sequence: | 201025762 | Sequence: | 201025763 | Sequence: | 201025764 | Sequence: | 201025765 | Sequence: | 201025766 | Sequence: | 201025767 | Sequence: | 201025768 | Sequence: | 201025769 | Sequence: | 201025770 | Sequence: | 201025771 | Sequence: | 201025772 | Sequence: | 201025773 | Sequence: | 201025774 | Sequence: | 201025775 | Sequence: | 201025776 | Sequence: | 201025777 | Sequence: | 201025778 | Sequence: | 201025779 | Sequence: | 201025780 |
Name | City of Hope ( Site 0002) | Name | Cedars Sinai Medical Center ( Site 0003) | Name | University of California Davis Comprehensive Cancer Center ( Site 0005) | Name | University of Colorado, Anschutz Cancer Pavilion ( Site 0007) | Name | University of Florida-Health Cancer Center-Orlando ( Site 0015) | Name | Rutgers Cancer Institute of New Jersey ( Site 0009) | Name | Laura and Isaac Perlmutter Cancer Center at NYU Langone Health ( Site 0023) | Name | Sanford Fargo Medical Center ( Site 0059) | Name | Lehigh Valley Hospital- Cedar Crest ( Site 0047) | Name | Sanford Cancer Center ( Site 0058) | Name | West Cancer Center – East Campus ( Site 0018) | Name | Mary Crowley Cancer Research Centers – Medical City Hospital ( Site 0049) | Name | Swedish Medical Center ( Site 0021) | Name | University of Wisconsin Carbone Cancer Center ( Site 0017) | Name | Fundacion Favaloro para la Docencia e Investigacion Medica ( Site 2106) | Name | Hospital Aleman ( Site 2100) | Name | Hospital Britanico de Buenos Aires ( Site 2109) | Name | Instituto de Oncologia de Rosario ( Site 2105) | Name | CEMIC ( Site 2104) | Name | IDIM Instituto de Diagnostico e Investigaciones Metabolicas ( Site 2101) | Name | Royal Brisbane and Women s Hospital ( Site 0901) | Name | Alfred Health ( Site 0902) | Name | Sir Charles Gairdner Hospital ( Site 0903) | Name | BC Cancer – Abbotsford ( Site 0200) | Name | CancerCare Manitoba ( Site 0201) | Name | Hamilton Health Sciences-Juravinski Cancer Centre ( Site 0208) | Name | Sunnybrook Research Institute ( Site 0207) | Name | Princess Margaret Cancer Centre ( Site 0202) | Name | Centre Hospitalier de l Universite de Montreal – CHUM ( Site 0210) | Name | CHU de Quebec Universite de Laval ( Site 0206) | Name | Centro Investigación del Cáncer James Lind ( Site 1203) | Name | Fundacion Arturo Lopez Perez ( Site 1201) | Name | Pontificia Universidad Catolica de Chile ( Site 1202) | Name | Hospital Clinico Universidad de Chile ( Site 1200) | Name | Fundacion Colombiana de Cancerologia Clinica Vida ( Site 1105) | Name | Instituto Nacional de Cancerologia E.S.E ( Site 1102) | Name | Oncologos del Occidente S.A. ( Site 1106) | Name | Fundacion Valle del Lili ( Site 1101) | Name | Centre Antoine Lacassagne ( Site 0404) | Name | Centre Leon Berard ( Site 0405) | Name | Institut Claudius Regaud IUCT Oncopole ( Site 0403) | Name | Centre Oscar Lambret ( Site 0401) | Name | Institut de Cancerologie de l Ouest Centre Rene Gauducheau ( Site 0402) | Name | Institut Gustave Roussy ( Site 0400) | Name | Robert Bosch GmbH ( Site 0307) | Name | Universitaetsklinikum Regensburg ( Site 0304) | Name | Universitaetsklinikum Frankfurt ( Site 0306) | Name | HELIOS Dr. Horst Schmidt Kliniken Wiesbaden ( Site 0301) | Name | SRH Wald-Klinikum Gera GmbH ( Site 0309) | Name | Universitaetsklinikum Jena ( Site 0302) | Name | Soroka Medical Center ( Site 0601) | Name | Rambam Medical Center ( Site 0602) | Name | Hadassah Ein Kerem Medical Center ( Site 0604) | Name | Chaim Sheba Medical Center ( Site 0600) | Name | Sourasky Medical Center ( Site 0603) | Name | Istituto Clinico Humanitas Research Hospital ( Site 1402) | Name | Policlinico Le Scotte – A.O. Senese ( Site 1401) | Name | Istituto Nazionale Tumori Fondazione Pascale ( Site 1400) | Name | Fondazione Policlinico Universitario A. Gemelli ( Site 1403) | Name | Asan Medical Center ( Site 1002) | Name | Seoul National University Hospital ( Site 1000) | Name | Severance Hospital Yonsei University Health System ( Site 1001) | Name | Arkhangelsk Clinical Oncological Dispensary ( Site 1600) | Name | Russian Oncological Research Center n.a. N.N. Blokhin ( Site 1604) | Name | Leningrad Regional Oncology Center ( Site 1609) | Name | Scientific Research Oncology Institute n.a. N.N.Petrov ( Site 1610) | Name | City Clinical Oncology Center ( Site 1608) | Name | Republican Clinical Oncology Dispensary of Tatarstan MoH ( Site 1603) | Name | Hospital Clinic i Provincial ( Site 0703) | Name | Hospital Universitario Gregorio Maranon ( Site 0701) | Name | Clinica Universitaria de Navarra ( Site 0704) | Name | Hospital Ramon y Cajal ( Site 0702) | Name | Inselspital Universitaetsspital Bern ( Site 1705) | Name | Kantonsspital Graubuenden ( Site 1704) | Name | Kantonsspital St. Gallen ( Site 1702) | Name | Ospedale Regionale di Bellinzona e Valli ( Site 1703) | Name | Hopitaux Universitaires de Geneve HUG ( Site 1701) | Name | Universitaetsspital Zurich ( Site 1700) | Name | National Cheng Kung University Hospital ( Site 3003) | Name | National Taiwan University Hospital ( Site 3000) | Name | Chulalongkorn University ( Site 5001) | Name | Ramathibodi Hospital. ( Site 5002) | Name | Siriraj Hospital ( Site 5003) | Name | Cambridge University Hospitals NHS Trust ( Site 0803) | Name | Leicester Royal Infirmary. Univ. Hosp. of Leicester NHS Trust ( Site 0804) | Name | Guy's Hospital ( Site 0806) | Name | Royal Marsden Hospital (Sutton) ( Site 0800) | Name | Christie NHS Foundation Trust ( Site 0805) |
City | Duarte | City | Los Angeles | City | Sacramento | City | Aurora | City | Orlando | City | New Brunswick | City | New York | City | Fargo | City | Allentown | City | Sioux Falls | City | Germantown | City | Dallas | City | Seattle | City | Madison | City | Ciudad Autonoma de Buenos Aires | City | Buenos Aires | City | Ciudad de Buenos Aires | City | Rosario | City | Buenos Aires | City | Caba | City | Herston | City | Melbourne | City | Nedlands | City | Abbotsford | City | Winnipeg | City | Hamilton | City | Toronto | City | Toronto | City | Montreal | City | Quebec | City | Temuco | City | Santiago | City | Santiago | City | Santiago | City | Medellin | City | Bogota | City | Pereira | City | Cali | City | Nice | City | Lyon | City | Toulouse | City | Lille | City | Saint-Herblain | City | Villejuif | City | Stuttgart | City | Regensburg | City | Frankfurt am Main | City | Wiesbaden | City | Gera | City | Jena | City | Beer Sheva | City | Haifa | City | Jerusalem | City | Ramat Gan | City | Tel Aviv | City | Rozzano | City | Siena | City | Napoli | City | Roma | City | Songpagu | City | Seoul | City | Seoul | City | Arkhangelsk | City | Moscow | City | Saint-Petersburg | City | Saint-Petersburg | City | Saint-Petersburg | City | Kazan | City | Barcelona | City | Madrid | City | Madrid | City | Madrid | City | Bern | City | Chur | City | St. Gallen | City | Bellinzona | City | Geneve | City | Zurich | City | Tainan | City | Taipei | City | Bangkok | City | Bangkok | City | Bangkok | City | Cambridge | City | Leicester | City | London | City | London | City | Manchester |
State | California | State | California | State | California | State | Colorado | State | Florida | State | New Jersey | State | New York | State | North Dakota | State | Pennsylvania | State | South Dakota | State | Tennessee | State | Texas | State | Washington | State | Wisconsin | State | Buenos Aires | State | Caba | State | Caba | State | Santa Fe | State | Queensland | State | Victoria | State | Western Australia | State | British Columbia | State | Manitoba | State | Ontario | State | Ontario | State | Ontario | State | Quebec | State | Araucania | State | Region M. De Santiago | State | Region M. De Santiago | State | Region M. De Santiago | State | Antioquia | State | Distrito Capital De Bogota | State | Risaralda | State | Valle Del Cauca | State | Alpes-Maritimes | State | Auvergne | State | Haute-Garonne | State | Nord | State | Val-de-Marne | State | Val-de-Marne | State | Baden-Wurttemberg | State | Bayern | State | Hessen | State | Hessen | State | Thuringen | State | Thuringen | State | Milano | State | Toscana | State | Seoul | State | Arkhangel Skaya Oblast | State | Moskva | State | Sankt-Peterburg | State | Sankt-Peterburg | State | Sankt-Peterburg | State | Tatarstan, Respublika | State | Berne | State | Grisons | State | Sankt Gallen | State | Ticino | State | Krung Thep Maha Nakhon | State | Krung Thep Maha Nakhon | State | Krung Thep Maha Nakhon | State | Cambridgeshire | State | Leicestershire | State | London, City Of | State | Surrey | ||||||||||||||||||||||||||||||||||||||||||
Zip | 91010 | Zip | 90048 | Zip | 95817 | Zip | 80045 | Zip | 32806 | Zip | 08901 | Zip | 10016 | Zip | 58102 | Zip | 18103 | Zip | 57104 | Zip | 38138 | Zip | 75230 | Zip | 98104 | Zip | 53792-0001 | Zip | C1078AAI | Zip | 1118 | Zip | C1280AEB | Zip | S2000KZE | Zip | C1431FWO | Zip | C1012AAR | Zip | 4029 | Zip | 3004 | Zip | 6009 | Zip | V2S 0C2 | Zip | R3E 0V9 | Zip | L8V 4X2 | Zip | M4N 3M5 | Zip | M5G 2M9 | Zip | H2X 3E4 | Zip | G1R 2J6 | Zip | 4780000 | Zip | 7500921 | Zip | 8330024 | Zip | 8380456 | Zip | 050030 | Zip | 110321 | Zip | 660001 | Zip | 760032 | Zip | 06189 | Zip | 69373 | Zip | 31059 | Zip | 59000 | Zip | 44805 | Zip | 94800 | Zip | 70376 | Zip | 93053 | Zip | 60528 | Zip | 65199 | Zip | 07548 | Zip | 07740 | Zip | 8457108 | Zip | 3109601 | Zip | 9112001 | Zip | 5262000 | Zip | 6423906 | Zip | 53100 | Zip | 80131 | Zip | 00168 | Zip | 05505 | Zip | 03080 | Zip | 03722 | Zip | 163045 | Zip | 115478 | Zip | 188663 | Zip | 197758 | Zip | 198255 | Zip | 420029 | Zip | 08036 | Zip | 28009 | Zip | 28027 | Zip | 28034 | Zip | 3010 | Zip | 7000 | Zip | 9007 | Zip | 6500 | Zip | 1211 | Zip | 8091 | Zip | 704 | Zip | 10002 | Zip | 10330 | Zip | 10400 | Zip | 10700 | Zip | CB2 0QQ | Zip | LE1 5WW | Zip | SE1 9RT | Zip | SM3 5PT | Zip | M20 4BX | ||
Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | Argentina | Country | Argentina | Country | Argentina | Country | Argentina | Country | Argentina | Country | Argentina | Country | Australia | Country | Australia | Country | Australia | Country | Canada | Country | Canada | Country | Canada | Country | Canada | Country | Canada | Country | Canada | Country | Canada | Country | Chile | Country | Chile | Country | Chile | Country | Chile | Country | Colombia | Country | Colombia | Country | Colombia | Country | Colombia | Country | France | Country | France | Country | France | Country | France | Country | France | Country | France | Country | Germany | Country | Germany | Country | Germany | Country | Germany | Country | Germany | Country | Germany | Country | Israel | Country | Israel | Country | Israel | Country | Israel | Country | Israel | Country | Italy | Country | Italy | Country | Italy | Country | Italy | Country | Korea, Republic of | Country | Korea, Republic of | Country | Korea, Republic of | Country | Russian Federation | Country | Russian Federation | Country | Russian Federation | Country | Russian Federation | Country | Russian Federation | Country | Russian Federation | Country | Spain | Country | Spain | Country | Spain | Country | Spain | Country | Switzerland | Country | Switzerland | Country | Switzerland | Country | Switzerland | Country | Switzerland | Country | Switzerland | Country | Taiwan | Country | Taiwan | Country | Thailand | Country | Thailand | Country | Thailand | Country | United Kingdom | Country | United Kingdom | Country | United Kingdom | Country | United Kingdom | Country | United Kingdom |
Browse Interventions
Sequence: | 96458967 | Sequence: | 96458968 | Sequence: | 96458969 | Sequence: | 96458970 | Sequence: | 96458971 | Sequence: | 96458972 | Sequence: | 96458973 | Sequence: | 96458974 |
Mesh Term | Pembrolizumab | Mesh Term | Lenvatinib | Mesh Term | Antineoplastic Agents, Immunological | Mesh Term | Antineoplastic Agents | Mesh Term | Immune Checkpoint Inhibitors | Mesh Term | Molecular Mechanisms of Pharmacological Action | Mesh Term | Protein Kinase Inhibitors | Mesh Term | Enzyme Inhibitors |
Downcase Mesh Term | pembrolizumab | Downcase Mesh Term | lenvatinib | Downcase Mesh Term | antineoplastic agents, immunological | Downcase Mesh Term | antineoplastic agents | Downcase Mesh Term | immune checkpoint inhibitors | Downcase Mesh Term | molecular mechanisms of pharmacological action | Downcase Mesh Term | protein kinase inhibitors | Downcase Mesh Term | enzyme inhibitors |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Conditions
Sequence: | 52429204 | Sequence: | 52429205 | Sequence: | 52429206 | Sequence: | 52429207 | Sequence: | 52429208 | Sequence: | 52429209 | Sequence: | 52429210 | Sequence: | 52429211 |
Name | Advanced Solid Tumors | Name | Triple Negative Breast Cancer | Name | Ovarian Cancer | Name | Gastric Cancer | Name | Colorectal Cancer | Name | Glioblastoma | Name | Biliary Tract Cancers | Name | Pancreatic Cancer |
Downcase Name | advanced solid tumors | Downcase Name | triple negative breast cancer | Downcase Name | ovarian cancer | Downcase Name | gastric cancer | Downcase Name | colorectal cancer | Downcase Name | glioblastoma | Downcase Name | biliary tract cancers | Downcase Name | pancreatic cancer |
Id Information
Sequence: | 40342086 | Sequence: | 40342087 | Sequence: | 40342088 | Sequence: | 40342089 | Sequence: | 40342090 |
Id Source | org_study_id | Id Source | secondary_id | Id Source | secondary_id | Id Source | secondary_id | Id Source | secondary_id |
Id Value | 7902-005 | Id Value | MK-7902-005 | Id Value | E7080-G000-224 | Id Value | LEAP-005 | Id Value | 2018-003747-37 |
Id Type | Other Identifier | Id Type | Other Identifier | Id Type | Other Identifier | Id Type | EudraCT Number | ||
Id Type Description | Merck Protocol Number | Id Type Description | Eisai Protocol Number | Id Type Description | Merck | ||||
Countries
Sequence: | 42773650 | Sequence: | 42773651 | Sequence: | 42773652 | Sequence: | 42773653 | Sequence: | 42773654 | Sequence: | 42773655 | Sequence: | 42773656 | Sequence: | 42773657 | Sequence: | 42773658 | Sequence: | 42773659 | Sequence: | 42773660 | Sequence: | 42773661 | Sequence: | 42773662 | Sequence: | 42773663 | Sequence: | 42773664 | Sequence: | 42773665 | Sequence: | 42773666 |
Name | United States | Name | Argentina | Name | Australia | Name | Canada | Name | Chile | Name | Colombia | Name | France | Name | Germany | Name | Israel | Name | Italy | Name | Korea, Republic of | Name | Russian Federation | Name | Spain | Name | Switzerland | Name | Taiwan | Name | Thailand | Name | United Kingdom |
Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False | Removed | False |
Design Groups
Sequence: | 55879552 | Sequence: | 55879553 |
Group Type | Experimental | Group Type | Experimental |
Title | Pembrolizumab + Lenvatinib (Arm 1) | Title | Lenvatinib Monotherapy (Arm 2) |
Description | Participants receive pembrolizumab 200 mg via intravenous (IV) infusion on Day 1 of each 21-day cycle (Q3W) plus lenvatinib 20 mg via oral capsule once a day (QD). Pembrolizumab will be administered for up to 35 cycles (up to 2 years). Lenvatinib will be administered until progressive disease or unacceptable toxicity (up to at least 2 years). | Description | Participants receive lenvatinib 24 mg via oral capsule QD, to be administered until progressive disease or unacceptable toxicity (up to at least 2 years). |
Interventions
Sequence: | 52738566 | Sequence: | 52738567 |
Intervention Type | Biological | Intervention Type | Drug |
Name | Pembrolizumab | Name | Lenvatinib |
Description | Administered as an IV infusion on Day 1 Q3W. | Description | Administered orally once a day during each 21-day cycle. |
Keywords
Sequence: | 80217521 | Sequence: | 80217522 | Sequence: | 80217523 | Sequence: | 80217524 | Sequence: | 80217525 | Sequence: | 80217526 | Sequence: | 80217527 | Sequence: | 80217528 |
Name | programmed cell death 1 (PD-1, PD1) | Name | programmed cell death ligand 1 (PD-L1, PDL1) | Name | programmed cell death ligand 2 (PD-L2, PDL2) | Name | tyrosine kinase inhibitor (TKI) | Name | multiple TKI | Name | Vascular Endothelial Growth Factor Receptor (VEFG) | Name | Fibroblast Growth Factor (FGF) | Name | Platelet-Derived Growth Factor (PDGF) |
Downcase Name | programmed cell death 1 (pd-1, pd1) | Downcase Name | programmed cell death ligand 1 (pd-l1, pdl1) | Downcase Name | programmed cell death ligand 2 (pd-l2, pdl2) | Downcase Name | tyrosine kinase inhibitor (tki) | Downcase Name | multiple tki | Downcase Name | vascular endothelial growth factor receptor (vefg) | Downcase Name | fibroblast growth factor (fgf) | Downcase Name | platelet-derived growth factor (pdgf) |
Design Outcomes
Sequence: | 178349302 | Sequence: | 178349303 | Sequence: | 178349304 | Sequence: | 178349305 | Sequence: | 178349306 | Sequence: | 178349307 | Sequence: | 178349308 | Sequence: | 178349309 | Sequence: | 178349310 | Sequence: | 178349311 | Sequence: | 178349312 | Sequence: | 178349313 | Sequence: | 178349314 | Sequence: | 178349315 | Sequence: | 178349316 | Sequence: | 178349317 | Sequence: | 178349318 | Sequence: | 178349319 | Sequence: | 178349320 | Sequence: | 178349321 |
Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Objective Response Rate (ORR) per Response Evaluation Criteria In Solid Tumors version 1.1 (RECIST 1.1) or Response Assessment in Neuro-Oncology (RANO) Criteria for Glioblastoma (GBM) by Investigator Assessment in Initial Cohorts | Measure | ORR per RECIST 1.1 or RANO (GBM) by Blinded Independent Central Review (BICR) in Expanded Cohorts (Combined with Initial Cohorts) | Measure | Percentage of Participants Receiving Pembrolizumab Plus Lenvatinib who Experience an Adverse Event (AE) | Measure | Percentage of Participants Receiving Pembrolizumab Plus Lenvatinib who Discontinue Study Treatment Due to an AE | Measure | Percentage of Participants Receiving Lenvatinib Monotherapy who Experience an AE | Measure | Percentage of Participants Receiving Lenvatinib Monotherapy who Discontinue Study Treatment Due to an Adverse Event (AE) | Measure | Disease Control Rate (DCR) per RECIST 1.1 by Investigator Assessment in Initial Cohorts | Measure | Duration of Response (DOR) per RECIST 1.1 or RANO (GBM) by Investigator Assessment in Initial Cohorts | Measure | Progression Free Survival (PFS) per RECIST 1.1 or RANO (GBM) by Investigator Assessment in Initial Cohorts | Measure | Overall Survival (OS) in Initial Cohorts | Measure | DCR per RECIST 1.1 by BICR in Expanded Cohorts (Combined with Initial Cohorts) | Measure | DOR per RECIST 1.1 or RANO (GBM) by BICR in Expanded Cohorts (Combined with Initial Cohorts) | Measure | PFS per RECIST 1.1 or RANO (GBM) by BICR in Expanded Cohorts (Combined with Initial Cohorts) | Measure | OS in Expanded Cohorts (Combined with Initial Cohorts) | Measure | ORR per RECIST 1.1 by BICR in Lenvatinib Monotherapy Arm | Measure | DCR per RECIST 1.1 by BICR in Lenvatinib Monotherapy Arm | Measure | DOR per RECIST 1.1 by BICR in Lenvatinib Monotherapy Arm | Measure | PFS per RECIST 1.1 by BICR in Lenvatinib Monotherapy Arm | Measure | OS in Lenvatinib Monotherapy Arm | Measure | Plasma Concentration of Lenvatinib |
Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Up to approximately 72 months | Time Frame | Cycle 1 Day 1: 0.5-4 hours and 6-10 hours post-dose; Cycle 1 Day 15: pre-dose and 2-12 hours post-dose; Cycle 2 Day 1: pre-dose, 0.5-4 hours, and 6-10 hours post-dose (up to approximately 23 days). Each cycle is 21 days. |
Description | ORR is defined as the percentage of participants who have a confirmed complete response (CR: disappearance of all target lesions) or partial response (PR: at least a 30% decrease in the sum of diameters [SOD] of target lesions, taking as reference the baseline SOD) as assessed by the investigator per RECIST 1.1, which is modified for this study to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ. For participants with GBM, response will be assessed by the investigator based on RANO criteria (CR: disappearance of all target lesions, PR: sum of products of diameters [SPD] decreased by ≥ 50% from baseline value). For participants in the pancreatic cancer cohort, response will be assessed by blinded independent central review (BICR). | Description | ORR is defined as the percentage of participants who have a confirmed CR (disappearance of all target lesions) or PR (at least a 30% decrease in the SOD of target lesions, taking as reference the baseline SOD) as assessed by BICR per RECIST 1.1, which is modified for this study to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ. For participants with GBM, response will be assessed based on RANO criteria (CR: disappearance of all target lesions, PR: SPD decreased by ≥ 50% from baseline value). | Description | An AE is any untoward medical occurrence in a clinical study participant that is temporally associated with the use of study treatment, whether or not considered related to the study treatment. The percentage of participants receiving pembrolizumab plus lenvatinib who experience at least one AE will be reported. | Description | An AE is any untoward medical occurrence in a clinical study participant that is temporally associated with the use of study treatment, whether or not considered related to the study treatment. The percentage of participants receiving pembrolizumab plus lenvatinib who discontinue study treatment due to an AE will be reported. | Description | An AE is any untoward medical occurrence in a clinical study participant that is temporally associated with the use of study treatment, whether or not considered related to the study treatment. The percentage of participants receiving lenvatinib monotherapy who experience at least one AE will be reported. | Description | An AE is any untoward medical occurrence in a clinical study participant that is temporally associated with the use of study treatment, whether or not considered related to the study treatment. The percentage of participants receiving lenvatinib monotherapy who discontinue study treatment due to an AE will be reported. | Description | DCR is defined as the percentage of participants who have a best overall response of CR, PR, or stable disease (SD) per RECIST 1.1. RECIST 1.1 has been modified for this study to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ. DCR will be assessed by the investigator for all initial cohorts except for the pancreatic cancer cohort, will be assessed by BICR. | Description | DOR is determined by disease assessment and is defined as the time from the earliest date of qualifying response until earliest date of disease progression or death from any cause, whichever comes first. RECIST 1.1 has been modified for this study to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ. DOR will be assessed by the investigator for all initial cohorts except for the pancreatic cancer cohort, will be assessed by BICR. | Description | PFS is defined as the time from date of study treatment to the first documented disease progression based on RECIST 1.1, modified to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ (or RANO for GBM participants), or death due to any cause, whichever occurs first. PFS will be assessed by the investigator for all initial cohorts except for the pancreatic cancer cohort, will be assessed by BICR. | Description | OS is defined as the time from the date of study treatment to the date of death due to any cause. | Description | DCR is defined as the percentage of participants who have a best overall response of CR, PR, or (SD) per RECIST 1.1. RECIST 1.1 has been modified for this study to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ, and will be assessed by BICR for this outcome measure. | Description | DOR is determined by disease assessment and is defined as the time from the earliest date of qualifying response until earliest date of disease progression or death from any cause, whichever comes first. RECIST 1.1 has been modified for this study to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ, and will be assessed by BICR for this outcome measure. | Description | PFS is defined as the time from date of study treatment to the first documented disease progression based on RECIST 1.1, modified to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ (or RANO for GBM participants), or death due to any cause, whichever occurs first, as assessed by BICR. | Description | OS is defined as the time from the date of study treatment to the date of death due to any cause. | Description | ORR is defined as the percentage of participants who have a confirmed CR (disappearance of all target lesions) or PR (at least a 30% decrease in the SOD of target lesions, taking as reference the baseline SOD) as assessed by BICR per RECIST 1.1, which is modified for this study to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ. | Description | DCR is defined as the percentage of participants who have a best overall response of CR, PR, or SD per RECIST 1.1. RECIST 1.1 has been modified for this study to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ, and will be assessed by BICR for this outcome measure. | Description | DOR is determined by disease assessment and is defined as the time from the earliest date of qualifying response until earliest date of disease progression or death from any cause, whichever comes first. RECIST 1.1 has been modified for this study to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ, and will be assessed by BICR for this outcome measure. | Description | PFS is defined as the time from date of study treatment to the first documented disease progression based on RECIST 1.1, modified to follow a maximum of 10 target lesions and a maximum of 5 target lesions per organ (or RANO for GBM participants), or death due to any cause, whichever occurs first, as assessed by BICR. | Description | OS is defined as the time from the date of study treatment to the date of death due to any cause. | Description | Blood samples will be obtained on Day 1 and Day 15 of Cycle 1 (21-day cycle) and Day 1 of Cycle 2 (21-day cycle) for pharmacokinetic (PK) analysis to determine the plasma concentration of lenvatinib. |
Browse Conditions
Sequence: | 194467972 | Sequence: | 194467973 | Sequence: | 194467974 | Sequence: | 194467975 | Sequence: | 194467976 | Sequence: | 194467977 | Sequence: | 194467978 | Sequence: | 194467979 | Sequence: | 194467980 | Sequence: | 194467981 | Sequence: | 194467982 | Sequence: | 194467983 | Sequence: | 194467984 | Sequence: | 194467985 | Sequence: | 194467986 | Sequence: | 194467987 | Sequence: | 194467988 | Sequence: | 194467989 | Sequence: | 194467990 |
Mesh Term | Glioblastoma | Mesh Term | Triple Negative Breast Neoplasms | Mesh Term | Biliary Tract Neoplasms | Mesh Term | Neoplasms | Mesh Term | Digestive System Neoplasms | Mesh Term | Neoplasms by Site | Mesh Term | Digestive System Diseases | Mesh Term | Astrocytoma | Mesh Term | Glioma | Mesh Term | Neoplasms, Neuroepithelial | Mesh Term | Neuroectodermal Tumors | Mesh Term | Neoplasms, Germ Cell and Embryonal | Mesh Term | Neoplasms by Histologic Type | Mesh Term | Neoplasms, Glandular and Epithelial | Mesh Term | Neoplasms, Nerve Tissue | Mesh Term | Breast Neoplasms | Mesh Term | Breast Diseases | Mesh Term | Skin Diseases | Mesh Term | Biliary Tract Diseases |
Downcase Mesh Term | glioblastoma | Downcase Mesh Term | triple negative breast neoplasms | Downcase Mesh Term | biliary tract neoplasms | Downcase Mesh Term | neoplasms | Downcase Mesh Term | digestive system neoplasms | Downcase Mesh Term | neoplasms by site | Downcase Mesh Term | digestive system diseases | Downcase Mesh Term | astrocytoma | Downcase Mesh Term | glioma | Downcase Mesh Term | neoplasms, neuroepithelial | Downcase Mesh Term | neuroectodermal tumors | Downcase Mesh Term | neoplasms, germ cell and embryonal | Downcase Mesh Term | neoplasms by histologic type | Downcase Mesh Term | neoplasms, glandular and epithelial | Downcase Mesh Term | neoplasms, nerve tissue | Downcase Mesh Term | breast neoplasms | Downcase Mesh Term | breast diseases | Downcase Mesh Term | skin diseases | Downcase Mesh Term | biliary tract diseases |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48558185 | Sequence: | 48558186 |
Agency Class | INDUSTRY | Agency Class | INDUSTRY |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator |
Name | Merck Sharp & Dohme LLC | Name | Eisai Inc. |
Overall Officials
Sequence: | 29419486 |
Role | Study Director |
Name | Medical Director |
Affiliation | Merck Sharp & Dohme LLC |
Design Group Interventions
Sequence: | 68501784 | Sequence: | 68501785 | Sequence: | 68501786 |
Design Group Id | 55879552 | Design Group Id | 55879553 | Design Group Id | 55879552 |
Intervention Id | 52738566 | Intervention Id | 52738567 | Intervention Id | 52738567 |
Eligibilities
Sequence: | 30913351 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Has a histologically or cytologically-documented, advanced (metastatic and/or unresectable) solid tumor that is incurable and for which prior standard systemic therapy has failed in one of the following cohorts: TNBC, Ovarian Cancer, Gastric Cancer, Colorectal Cancer, GBM, BTC (intrahepatic, extrahepatic cholangiocarcinoma and gall bladder cancer; excludes Ampulla of Vater), Pancreatic Cancer For Triple Negative Breast Cancer Participants: Has received one or 2 prior lines of therapy For Ovarian Cancer Participants: – Has primary ovarian cancer and has received 3 prior lines of therapy. For Gastric Cancer Participants: – Has received 2 prior lines of therapy. Note: Gastric cancer will include participants with both gastric and gastroesophageal junction (GEJ) adenocarcinoma. Participants with squamous cell carcinoma histology are not eligible For Colorectal Cancer Participants: – Has received 2 prior lines of therapy For GBM Participants: Has failed initial systemic therapy for newly diagnosed GBM For Biliary Tract Cancer Participants: Has received 1 prior line of therapy For Pancreatic Cancer Participants: Has pathologically (histologically or cytologically) confirmed pancreatic ductal adenocarcinoma that is metastatic at enrollment Exclusion Criteria: Has gastrointestinal malabsorption or any other condition that might affect the absorption of lenvatinib For GBM Participants: Has carcinomatous meningitis |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254176392 |
Number Of Facilities | 88 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | False |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 6 |
Number Of Secondary Outcomes To Measure | 14 |
Designs
Sequence: | 30659046 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | None (Open Label) |
Intervention Other Names
Sequence: | 26800394 | Sequence: | 26800395 | Sequence: | 26800396 | Sequence: | 26800397 | Sequence: | 26800398 |
Intervention Id | 52738566 | Intervention Id | 52738566 | Intervention Id | 52738567 | Intervention Id | 52738567 | Intervention Id | 52738567 |
Name | MK-3475 | Name | Keytruda® | Name | MK-7902 | Name | E7080 | Name | LENVIMA™ |
Links
Sequence: | 4407745 |
Url | http://merckoncologyclinicaltrials.com |
Description | Merck Oncology Clinical Trial Information |
Responsible Parties
Sequence: | 29025720 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797313
2019-01-22
https://zephyrnet.com/?p=NCT03797313
NCT03797313https://www.clinicaltrials.gov/study/NCT03797313?tab=tableNANANAThis is an observational cohort study of the association between patient expectations for functional recovery and quality of life among acute respiratory failure survivors 6 months after hospital discharge.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2021-12-15 |
Start Month Year | January 22, 2019 |
Primary Completion Month Year | December 1, 2021 |
Verification Month Year | February 2021 |
Verification Date | 2021-02-28 |
Last Update Posted Date | 2021-12-15 |
Detailed Descriptions
Sequence: | 20774584 |
Description | This study will enroll adults who are diagnosed with acute respiratory failure during an ICU admission and discharged from the ICU alive. All participants will receive usual clinical care. Participant expectations for functional recovery will be assessed before hospital discharge via a standardized questionnaire containing a visual analogue scale and questions about expected ability and importance of being able to perform activities of daily living and instrumental activities of daily living in 6 months. At 6 months, participants will be re-contacted by phone. Study staff will administer questionnaires to assess whether patient expectations have been met. Quality of life will be assessed using the WHOQOL-BREF and the EQ-5D-VAS. |
Facilities
Sequence: | 200548214 | Sequence: | 200548215 | Sequence: | 200548216 | Sequence: | 200548217 |
Name | Johns Hopkins University | Name | Beth Israel Deaconess Medical Center | Name | Vanderbilt University | Name | Intermountain Medical Center |
City | Baltimore | City | Boston | City | Nashville | City | Murray |
State | Maryland | State | Massachusetts | State | Tennessee | State | Utah |
Zip | 21287 | Zip | 02215 | Zip | 37235 | Zip | 84107 |
Country | United States | Country | United States | Country | United States | Country | United States |
Conditions
Sequence: | 52306590 | Sequence: | 52306591 |
Name | Acute Respiratory Failure | Name | Post Intensive Care Syndrome |
Downcase Name | acute respiratory failure | Downcase Name | post intensive care syndrome |
Id Information
Sequence: | 40255942 | Sequence: | 40255943 | Sequence: | 40255944 |
Id Source | org_study_id | Id Source | secondary_id | Id Source | secondary_id |
Id Value | IRB00197235 | Id Value | 00181895 | Id Value | K01HL141637-01 |
Id Type | Other Identifier | Id Type | U.S. NIH Grant/Contract | ||
Id Type Description | Other | ||||
Id Link | https://reporter.nih.gov/quickSearch/K01HL141637-01 |
Countries
Sequence: | 42674764 |
Name | United States |
Removed | False |
Design Groups
Sequence: | 55744516 | Sequence: | 55744517 |
Title | Patient's expectations met at Hospital discharge | Title | Patient's with unmet expectations at Hospital Discharge |
Description | ARF survivors whose expectations for recovery at hospital discharge are fully met 6 months later. | Description | ARF survivors whose expectations for recovery at hospital discharge are not fully met 6 months later. |
Design Outcomes
Sequence: | 177878415 | Sequence: | 177878416 |
Outcome Type | primary | Outcome Type | secondary |
Measure | Quality of life measured using the World Health Organization Quality of Life-BREF instrument (WHOQOL-BREF) after hospital discharge | Measure | Patient expectation error measure using EQ-5D VAS |
Time Frame | 6 months after hospital discharge | Time Frame | 6 months after hospital discharge |
Description | WHOQOL-BREF is a measure of overall quality of life that evaluates satisfaction with important aspects of life rather than of health. The instrument contains 26 items across 4 domains, and requires approximately 5 minutes to administer over the phone. The 26 items in the WHOQOL-BREF are scored in four domains: physical, psychological, social relations, and environment, with between 3 and 8 items in each domain and two "benchmark" items addressing overall QoL. Transforming the raw scores results in a domain score between 0 – 100, enabling comparisons between domains with different numbers of items. Higher scores indicate greater participant satisfaction with their quality of life and lower scores indicate worse satisfaction with quality of life. | Description | A secondary analysis will estimate patient expectation error, defined as the difference between the health-related quality of life score expected at hospital discharge and the actual health related quality of life score assessed using the EQ-5D VAS 6 months after hospital discharge. The EQ-5D VAS ranges from 0 to 100 with 0 representing the worst imaginable health state and 100 representing the best imaginable health state. |
Browse Conditions
Sequence: | 194004048 | Sequence: | 194004049 | Sequence: | 194004050 | Sequence: | 194004051 | Sequence: | 194004052 |
Mesh Term | Respiratory Insufficiency | Mesh Term | Respiratory Distress Syndrome | Mesh Term | Respiration Disorders | Mesh Term | Respiratory Tract Diseases | Mesh Term | Lung Diseases |
Downcase Mesh Term | respiratory insufficiency | Downcase Mesh Term | respiratory distress syndrome | Downcase Mesh Term | respiration disorders | Downcase Mesh Term | respiratory tract diseases | Downcase Mesh Term | lung diseases |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48446356 | Sequence: | 48446357 |
Agency Class | OTHER | Agency Class | NIH |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator |
Name | Johns Hopkins University | Name | National Heart, Lung, and Blood Institute (NHLBI) |
Overall Officials
Sequence: | 29358082 |
Role | Principal Investigator |
Name | Alison Turnbull |
Affiliation | Johns Hopkins University |
Eligibilities
Sequence: | 30844061 |
Sampling Method | Non-Probability Sample |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Population | survivors of acute respiratory failure (ARF) who are expected to be discharged home alive. |
Criteria | Inclusion Criteria:
Age ≥ 18 years High flow nasal cannula with FIO2 ≥ 0.5 and flow rate ≥ 30 LPM for ≥ 24 consecutive hours* *Occasional rest periods of ≤ 1 hour each are not deducted from the calculation of consecutive hours. Expected by the clinical team to be discharged home alive Exclusion Criteria: Patient in ICU < 24 hours |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254193084 |
Number Of Facilities | 4 |
Registered In Calendar Year | 2019 |
Actual Duration | 34 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | False |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 1 |
Designs
Sequence: | 30589932 |
Observational Model | Cohort |
Time Perspective | Prospective |
Responsible Parties
Sequence: | 28956380 |
Responsible Party Type | Sponsor |
Study References
Sequence: | 52208856 | Sequence: | 52208857 | Sequence: | 52208858 | Sequence: | 52208859 | Sequence: | 52208860 | Sequence: | 52208861 | Sequence: | 52208862 | Sequence: | 52208863 | Sequence: | 52208864 | Sequence: | 52208865 | Sequence: | 52208866 | Sequence: | 52208867 | Sequence: | 52208868 | Sequence: | 52208869 | Sequence: | 52208870 | Sequence: | 52208871 | Sequence: | 52208872 | Sequence: | 52208873 | Sequence: | 52208874 | Sequence: | 52208875 | Sequence: | 52208876 | Sequence: | 52208877 | Sequence: | 52208878 | Sequence: | 52208879 | Sequence: | 52208880 | Sequence: | 52208881 | Sequence: | 52208882 | Sequence: | 52208883 | Sequence: | 52208884 |
Pmid | 16236739 | Pmid | 19865004 | Pmid | 20224063 | Pmid | 18263687 | Pmid | 19011152 | Pmid | 21946660 | Pmid | 28463657 | Pmid | 28448162 | Pmid | 21965016 | Pmid | 24160906 | Pmid | 19770733 | Pmid | 27632675 | Pmid | 27294981 | Pmid | 7655809 | Pmid | 20088892 | Pmid | 21629159 | Pmid | 23575998 | Pmid | 27622598 | Pmid | 24787107 | Pmid | 30160803 | Pmid | 5420677 | Pmid | 5349366 | Pmid | 14754765 | Pmid | 12964174 | Pmid | 26821587 | Pmid | 15085902 | Pmid | 2280326 | Pmid | 28395702 | Pmid | 25531451 |
Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background |
Citation | Rubenfeld GD, Caldwell E, Peabody E, Weaver J, Martin DP, Neff M, Stern EJ, Hudson LD. Incidence and outcomes of acute lung injury. N Engl J Med. 2005 Oct 20;353(16):1685-93. doi: 10.1056/NEJMoa050333. | Citation | Cox CE, Docherty SL, Brandon DH, Whaley C, Attix DK, Clay AS, Dore DV, Hough CL, White DB, Tulsky JA. Surviving critical illness: acute respiratory distress syndrome as experienced by patients and their caregivers. Crit Care Med. 2009 Oct;37(10):2702-8. doi: 10.1097/CCM.0b013e3181b6f64a. | Citation | Spragg RG, Bernard GR, Checkley W, Curtis JR, Gajic O, Guyatt G, Hall J, Israel E, Jain M, Needham DM, Randolph AG, Rubenfeld GD, Schoenfeld D, Thompson BT, Ware LB, Young D, Harabin AL. Beyond mortality: future clinical research in acute lung injury. Am J Respir Crit Care Med. 2010 May 15;181(10):1121-7. doi: 10.1164/rccm.201001-0024WS. Epub 2010 Mar 11. | Citation | Zambon M, Vincent JL. Mortality rates for patients with acute lung injury/ARDS have decreased over time. Chest. 2008 May;133(5):1120-7. doi: 10.1378/chest.07-2134. Epub 2008 Feb 8. | Citation | Phua J, Badia JR, Adhikari NK, Friedrich JO, Fowler RA, Singh JM, Scales DC, Stather DR, Li A, Jones A, Gattas DJ, Hallett D, Tomlinson G, Stewart TE, Ferguson ND. Has mortality from acute respiratory distress syndrome decreased over time?: A systematic review. Am J Respir Crit Care Med. 2009 Feb 1;179(3):220-7. doi: 10.1164/rccm.200805-722OC. Epub 2008 Nov 14. | Citation | Needham DM, Davidson J, Cohen H, Hopkins RO, Weinert C, Wunsch H, Zawistowski C, Bemis-Dougherty A, Berney SC, Bienvenu OJ, Brady SL, Brodsky MB, Denehy L, Elliott D, Flatley C, Harabin AL, Jones C, Louis D, Meltzer W, Muldoon SR, Palmer JB, Perme C, Robinson M, Schmidt DM, Scruth E, Spill GR, Storey CP, Render M, Votto J, Harvey MA. Improving long-term outcomes after discharge from intensive care unit: report from a stakeholders' conference. Crit Care Med. 2012 Feb;40(2):502-9. doi: 10.1097/CCM.0b013e318232da75. | Citation | Hopkins RO, Suchyta MR, Kamdar BB, Darowski E, Jackson JC, Needham DM. Instrumental Activities of Daily Living after Critical Illness: A Systematic Review. Ann Am Thorac Soc. 2017 Aug;14(8):1332-1343. doi: 10.1513/AnnalsATS.201701-059SR. | Citation | Kamdar BB, Huang M, Dinglas VD, Colantuoni E, von Wachter TM, Hopkins RO, Needham DM; National Heart, Lung, and Blood Institute Acute Respiratory Distress Syndrome Network. Joblessness and Lost Earnings after Acute Respiratory Distress Syndrome in a 1-Year National Multicenter Study. Am J Respir Crit Care Med. 2017 Oct 15;196(8):1012-1020. doi: 10.1164/rccm.201611-2327OC. | Citation | Lieu TA, Au D, Krishnan JA, Moss M, Selker H, Harabin A, Taggart V, Connors A; Comparative Effectiveness Research in Lung Diseases Workshop Panel. Comparative effectiveness research in lung diseases and sleep disorders: recommendations from the National Heart, Lung, and Blood Institute workshop. Am J Respir Crit Care Med. 2011 Oct 1;184(7):848-56. doi: 10.1164/rccm.201104-0634WS. | Citation | Carson SS, Goss CH, Patel SR, Anzueto A, Au DH, Elborn S, Gerald JK, Gerald LB, Kahn JM, Malhotra A, Mularski RA, Riekert KA, Rubenfeld GD, Weaver TE, Krishnan JA; American Thoracic Society Comparative Effectiveness Research Working Group. An official American Thoracic Society research statement: comparative effectiveness research in pulmonary, critical care, and sleep medicine. Am J Respir Crit Care Med. 2013 Nov 15;188(10):1253-61. doi: 10.1164/rccm.201310-1790ST. | Citation | Cox CE, Martinu T, Sathy SJ, Clay AS, Chia J, Gray AL, Olsen MK, Govert JA, Carson SS, Tulsky JA. Expectations and outcomes of prolonged mechanical ventilation. Crit Care Med. 2009 Nov;37(11):2888-94; quiz 2904. doi: 10.1097/CCM.0b013e3181ab86ed. | Citation | Lamas DJ, Owens RL, Nace RN, Massaro AF, Pertsch NJ, Gass J, Bernacki RE, Block SD. Opening the Door: The Experience of Chronic Critical Illness in a Long-Term Acute Care Hospital. Crit Care Med. 2017 Apr;45(4):e357-e362. doi: 10.1097/CCM.0000000000002094. | Citation | Turnbull AE, Davis WE, Needham DM, White DB, Eakin MN. Intensivist-reported Facilitators and Barriers to Discussing Post-Discharge Outcomes with Intensive Care Unit Surrogates. A Qualitative Study. Ann Am Thorac Soc. 2016 Sep;13(9):1546-52. doi: 10.1513/AnnalsATS.201603-212OC. | Citation | Thompson AG, Sunol R. Expectations as determinants of patient satisfaction: concepts, theory and evidence. Int J Qual Health Care. 1995 Jun;7(2):127-41. doi: 10.1093/intqhc/7.2.127. | Citation | Gonzalez Saenz de Tejada M, Escobar A, Herrera C, Garcia L, Aizpuru F, Sarasqueta C. Patient expectations and health-related quality of life outcomes following total joint replacement. Value Health. 2010 Jun-Jul;13(4):447-54. doi: 10.1111/j.1524-4733.2009.00685.x. Epub 2010 Jan 15. | Citation | Soroceanu A, Ching A, Abdu W, McGuire K. Relationship between preoperative expectations, satisfaction, and functional outcomes in patients undergoing lumbar and cervical spine surgery: a multicenter study. Spine (Phila Pa 1976). 2012 Jan 15;37(2):E103-8. doi: 10.1097/BRS.0b013e3182245c1f. | Citation | Hamilton DF, Lane JV, Gaston P, Patton JT, Macdonald D, Simpson AH, Howie CR. What determines patient satisfaction with surgery? A prospective cohort study of 4709 patients following total joint replacement. BMJ Open. 2013 Apr 9;3(4):e002525. doi: 10.1136/bmjopen-2012-002525. Print 2013. | Citation | Pihl K, Roos EM, Nissen N, JoRgensen U, Schjerning J, Thorlund JB. Over-optimistic patient expectations of recovery and leisure activities after arthroscopic meniscus surgery. Acta Orthop. 2016 Dec;87(6):615-621. doi: 10.1080/17453674.2016.1228411. Epub 2016 Sep 13. | Citation | Waljee J, McGlinn EP, Sears ED, Chung KC. Patient expectations and patient-reported outcomes in surgery: a systematic review. Surgery. 2014 May;155(5):799-808. doi: 10.1016/j.surg.2013.12.015. Epub 2013 Dec 16. | Citation | Aversa M, Chowdhury NA, Tomlinson G, Singer LG. Preoperative expectations for health-related quality of life after lung transplant. Clin Transplant. 2018 Oct;32(10):e13394. doi: 10.1111/ctr.13394. Epub 2018 Sep 25. | Citation | Katz S, Downs TD, Cash HR, Grotz RC. Progress in development of the index of ADL. Gerontologist. 1970 Spring;10(1):20-30. doi: 10.1093/geront/10.1_part_1.20. No abstract available. | Citation | Lawton MP, Brody EM. Assessment of older people: self-maintaining and instrumental activities of daily living. Gerontologist. 1969 Autumn;9(3):179-86. No abstract available. | Citation | Charney DS. Psychobiological mechanisms of resilience and vulnerability: implications for successful adaptation to extreme stress. Am J Psychiatry. 2004 Feb;161(2):195-216. doi: 10.1176/appi.ajp.161.2.195. | Citation | Connor KM, Davidson JR. Development of a new resilience scale: the Connor-Davidson Resilience Scale (CD-RISC). Depress Anxiety. 2003;18(2):76-82. doi: 10.1002/da.10113. | Citation | Cosco TD, Kaushal A, Richards M, Kuh D, Stafford M. Resilience measurement in later life: a systematic review and psychometric analysis. Health Qual Life Outcomes. 2016 Jan 28;14:16. doi: 10.1186/s12955-016-0418-6. | Citation | Skevington SM, Lotfy M, O'Connell KA; WHOQOL Group. The World Health Organization's WHOQOL-BREF quality of life assessment: psychometric properties and results of the international field trial. A report from the WHOQOL group. Qual Life Res. 2004 Mar;13(2):299-310. doi: 10.1023/B:QURE.0000018486.91360.00. | Citation | Zimet GD, Powell SS, Farley GK, Werkman S, Berkoff KA. Psychometric characteristics of the Multidimensional Scale of Perceived Social Support. J Pers Assess. 1990 Winter;55(3-4):610-7. doi: 10.1080/00223891.1990.9674095. | Citation | Shumaker SC, Frazier SK, Moser DK, Chung ML. Psychometric Properties of the Multidimensional Scale of Perceived Social Support in Patients With Heart Failure. J Nurs Meas. 2017 Apr 1;25(1):90-102. doi: 10.1891/1061-3749.25.1.90. | Citation | Hoffmann TC, Del Mar C. Patients' expectations of the benefits and harms of treatments, screening, and tests: a systematic review. JAMA Intern Med. 2015 Feb;175(2):274-86. doi: 10.1001/jamainternmed.2014.6016. |
]]>
https://zephyrnet.com/NCT03797300
2018-12-12
https://zephyrnet.com/?p=NCT03797300
NCT03797300https://www.clinicaltrials.gov/study/NCT03797300?tab=tableNANANAAssessment of Spry Health’s Loop oximetry accuracy in profound hypoxia Assessment of Spry Health’s Respiratory rate accuracy in normal conditions and profound hypoxia
<![CDATA[
Studies
Study First Submitted Date | 2019-01-02 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-01-09 |
Start Month Year | December 12, 2018 |
Primary Completion Month Year | December 14, 2018 |
Verification Month Year | January 2019 |
Verification Date | 2019-01-31 |
Last Update Posted Date | 2019-01-09 |
Facilities
Sequence: | 200053339 |
Name | UCSF Hypoxia Lab |
City | San Francisco |
State | California |
Zip | 94143 |
Country | United States |
Conditions
Sequence: | 52156526 | Sequence: | 52156527 | Sequence: | 52156528 |
Name | Hypoxia | Name | Hypercapnia | Name | Hypocapnia |
Downcase Name | hypoxia | Downcase Name | hypercapnia | Downcase Name | hypocapnia |
Id Information
Sequence: | 40148232 |
Id Source | org_study_id |
Id Value | SpryUCSF2 |
Countries
Sequence: | 42557765 |
Name | United States |
Removed | False |
Design Groups
Sequence: | 55577932 |
Group Type | Experimental |
Title | Primary |
Interventions
Sequence: | 52472032 |
Intervention Type | Device |
Name | Spry Loop Band |
Description | Loop band measures pulse oximetry and respiration rate |
Design Outcomes
Sequence: | 177328082 | Sequence: | 177328083 |
Outcome Type | primary | Outcome Type | primary |
Measure | Accuracy of SpO2 measurement | Measure | Accuracy of Respiratory Rate measurement |
Time Frame | duration of subject monitoring, usually up to one hour | Time Frame | duration of subject monitoring, usually up to one hour |
Description | Pulse oximetry measurement accuracy vs. gold standard | Description | Respiratory rate measurement accuracy vs. gold standard |
Browse Conditions
Sequence: | 193432165 | Sequence: | 193432166 | Sequence: | 193432167 | Sequence: | 193432168 |
Mesh Term | Hypoxia | Mesh Term | Hypercapnia | Mesh Term | Hypocapnia | Mesh Term | Signs and Symptoms, Respiratory |
Downcase Mesh Term | hypoxia | Downcase Mesh Term | hypercapnia | Downcase Mesh Term | hypocapnia | Downcase Mesh Term | signs and symptoms, respiratory |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48306107 | Sequence: | 48306108 |
Agency Class | INDUSTRY | Agency Class | OTHER |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator |
Name | Spry Health | Name | University of California, San Francisco |
Design Group Interventions
Sequence: | 68130895 |
Design Group Id | 55577932 |
Intervention Id | 52472032 |
Eligibilities
Sequence: | 30757373 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 60 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
Healthy adult willing to participate Exclusion Criteria: Wrist size outside the indicated use |
Adult | True |
Child | False |
Older Adult | False |
Calculated Values
Sequence: | 254228117 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Actual Duration | 0 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 60 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 2 |
Designs
Sequence: | 30503598 |
Allocation | N/A |
Intervention Model | Single Group Assignment |
Observational Model | |
Primary Purpose | Basic Science |
Time Perspective | |
Masking | None (Open Label) |
Responsible Parties
Sequence: | 28869876 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797287
2020-02-01
https://zephyrnet.com/?p=NCT03797287
NCT03797287https://www.clinicaltrials.gov/study/NCT03797287?tab=tableNANANAThis study will compare arthroscopic transosseous versus anchored rotator cuff repairs in terms of clinical outcomes, rotator cuff integrity, and cost-effectiveness. With the collection of patient-reported outcomes the health of patients undergoing each rotator cuff repair technique will be assessed. The aims of this study will be achieved through a clinical randomized controlled trial and a cost-effectiveness analysis.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-05-30 |
Start Month Year | February 1, 2020 |
Primary Completion Month Year | December 2025 |
Verification Month Year | May 2019 |
Verification Date | 2019-05-31 |
Last Update Posted Date | 2019-05-30 |
Detailed Descriptions
Sequence: | 20735953 |
Description | Study Design: After the decision to proceed with arthroscopic rotator cuff repair, patients will be asked to participate in this prospective randomized clinical trial.
Study Procedures: Before Surgery: The Informed Consent process will be completed prior to any data collection. Consent will be completed after explanation of each treatment group and the data to be collected. Baseline and demographic data will be collected prior to surgery: Randomization: Subjects will be randomized prior to surgery into one of the two rotator cuff repair technique groups using REDCap software. Randomization will be stratified by gender. Patient Visits: Patients will complete their questionnaires and testing before surgery then within 2 weeks, 3 months, 6 months, 1 year, and 2 years After the first week of surgery, patients will be given a pain diary to record all narcotic pain medications they consume during the 1st week post-op. An ultrasound will be done during their 6 month, 1 year, and 2 year follow up. |
Facilities
Sequence: | 200245101 |
Name | Johns Hopkins |
City | Columbia |
State | Maryland |
Zip | 21044 |
Country | United States |
Conditions
Sequence: | 52208532 | Sequence: | 52208533 | Sequence: | 52208534 | Sequence: | 52208535 |
Name | Shoulder Pain Chronic | Name | Shoulder Pain | Name | Rotator Cuff Tear | Name | Rotator Cuff Injury |
Downcase Name | shoulder pain chronic | Downcase Name | shoulder pain | Downcase Name | rotator cuff tear | Downcase Name | rotator cuff injury |
Id Information
Sequence: | 40186462 |
Id Source | org_study_id |
Id Value | IRB00046834 |
Countries
Sequence: | 42599953 |
Name | United States |
Removed | False |
Design Groups
Sequence: | 55635150 | Sequence: | 55635151 |
Group Type | Experimental | Group Type | Active Comparator |
Title | Tensor Tunnler | Title | Smith and Nephew PEEK Helicoil Anchor |
Description | The Tensor Tunneler (Chattanooga, TN) will be used to create the bone tunnels during the arthroscopic procedure. This is an FDA approved device and is used currently in routine clinical practice. | Description | The anchors used in this trial are FDA approved and are used currently in routine clinical practice (Anchor Rotator Cuff Repair). |
Interventions
Sequence: | 52522488 | Sequence: | 52522489 |
Intervention Type | Device | Intervention Type | Procedure |
Name | Tensor Tunnler | Name | Anchor Rotator Cuff Repair |
Description | Create the bone tunnels during the arthroscopic rotator cuff repair procedure | Description | The suture anchors (Smith and Nephew PEEK Helicoil Anchor) are inserted in bone and the sutures are then used to sew the tendons to bone arthroscopically. |
Design Outcomes
Sequence: | 177512865 | Sequence: | 177512866 | Sequence: | 177512867 | Sequence: | 177512868 | Sequence: | 177512869 | Sequence: | 177512870 | Sequence: | 177512871 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Change in condition of the shoulder as assessed by American Shoulder and Elbow Surgeon (ASES) Score | Measure | Change in shoulder pain as assessed by Visual Analog Pain Score | Measure | Change in Range of Motion (ROM) | Measure | Change in Strength Testing | Measure | Change in quality of life as assessed by the Western Ontario Rotator Cuff (WORC) Index | Measure | Change in health related quality of life as assessed by Short-Form Six-Dimension (SF-6D) | Measure | Implant Cost |
Time Frame | Before surgery, 2 weeks, 3 months, 6 months, and 1 year after surgery | Time Frame | Before surgery, 2 weeks, 3 months, 6 months, and 1 year after surgery | Time Frame | Before surgery, within 1 month after surgery, 3 months, 6 months, 1 year | Time Frame | Before surgery, 2 weeks, 3 months, 6 months, and 1 year after surgery | Time Frame | Before surgery, 1 year after surgery, 2 years after surgery | Time Frame | Before surgery, 2 weeks, 3 months, 6 months, and 1 year after surgery | Time Frame | Within 1 month after surgery |
Description | 10 separate questions is scored on an ordinal scale from 0-3 for a maximal raw functional score of 30 (no difficulties). | Description | Patients are asked to identify whether they are having pain in the shoulder and are asked to record the location of their pain on a 10 cm line that ranges from 0(no pain at all) to 10 (pain as bad as it can be) | Description | Total (combined glenohumeral and scapulothoracic) shoulder motion is measured. Both active and passive motion for both shoulders is recorded. Forward elevation is measured as the maximum arm-trunk angle viewed from any direction. External rotation is measured with the arm comfortably at the side and also with the arm at 90° of abduction. Internal rotation is measured by noting the highest segment of spinal anatomy reached with the thumb. Cross-body adduction is measured by measuring the distance of the antecubital fossa from the opposite acromion. | Description | Strength is graded according to the Medical Research Council grade. Strength is measured in forward elevation, abduction, external rotation with the arm comfortably at the side, and internal rotation with the arm comfortably at the side. A perfect score is a 5 in each category. | Description | Quality of Life Measurement tool for patients with rotator cuff disease where patients mark a line on 21 visual analogue scale (VAS) lines labeled 0 (not affected) – 100 (affected). These items will ask about physical symptoms, sports and recreation, work, social function, and emotions. The maximum score is 2100 for worst possible symptoms and 0 represents no symptoms at all. | Description | Measures of health related quality of life (HRQoL) using 11 items from the SF-36 or SF-12. Patients are asked about their physical functioning, role limitations, social functioning, pain, mental health, and vitality. A score of 1 represents full health. | Description | Review of costs through our billing department |
Browse Conditions
Sequence: | 193628731 | Sequence: | 193628732 | Sequence: | 193628733 | Sequence: | 193628734 | Sequence: | 193628735 | Sequence: | 193628736 | Sequence: | 193628737 | Sequence: | 193628738 | Sequence: | 193628739 | Sequence: | 193628740 | Sequence: | 193628741 |
Mesh Term | Shoulder Pain | Mesh Term | Rotator Cuff Injuries | Mesh Term | Arthralgia | Mesh Term | Joint Diseases | Mesh Term | Musculoskeletal Diseases | Mesh Term | Pain | Mesh Term | Neurologic Manifestations | Mesh Term | Rupture | Mesh Term | Wounds and Injuries | Mesh Term | Shoulder Injuries | Mesh Term | Tendon Injuries |
Downcase Mesh Term | shoulder pain | Downcase Mesh Term | rotator cuff injuries | Downcase Mesh Term | arthralgia | Downcase Mesh Term | joint diseases | Downcase Mesh Term | musculoskeletal diseases | Downcase Mesh Term | pain | Downcase Mesh Term | neurologic manifestations | Downcase Mesh Term | rupture | Downcase Mesh Term | wounds and injuries | Downcase Mesh Term | shoulder injuries | Downcase Mesh Term | tendon injuries |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48354144 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Johns Hopkins University |
Overall Officials
Sequence: | 29306219 |
Role | Principal Investigator |
Name | Uma Srikumaran, MD, MBA |
Affiliation | Johns Hopkins University |
Design Group Interventions
Sequence: | 68199752 | Sequence: | 68199753 |
Design Group Id | 55635150 | Design Group Id | 55635151 |
Intervention Id | 52522488 | Intervention Id | 52522489 |
Eligibilities
Sequence: | 30787125 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 75 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
Adults age 18-75 years old Exclusion Criteria: Patients with partial tears, massive rotator cuff tears that are irreparable, isolated subscapularis tears, and associated pathology (advanced degenerative changes) |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 253990069 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 75 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 6 |
Designs
Sequence: | 30533195 |
Allocation | Randomized |
Intervention Model | Parallel Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | Single |
Outcomes Assessor Masked | True |
Responsible Parties
Sequence: | 28899487 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797274
2019-02-08
https://zephyrnet.com/?p=NCT03797274
NCT03797274https://www.clinicaltrials.gov/study/NCT03797274?tab=tableNANANAMost drugs used in general anesthesia work on various receptors in the human brain, causing unconsciousness, loss of memory, and loss of reflection of the autonomic nervous system. After the anesthesia, baseline physiological function will be attained by administration of some reversal drugs or as the time goes by. In this process, various side effects may occur.
Emergence delirium (ED) is a representative behavioral disturbance after general anesthesia in children and that can cause several problems during the recovery period. Previous EEG studies reported that this phenomenon is related to hyperexcitation of the brain, and occurrence of epileptiform discharges during anesthesia induction may indicate an increased vulnerability for the development of a functional brain disorder in these children.
However, to the best of our knowledge, there is no studies concern evaluating quantitative EEG parameters for prediction of this postoperative negative behavior in children.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-05 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-09-04 |
Start Month Year | February 8, 2019 |
Primary Completion Month Year | May 29, 2019 |
Verification Month Year | September 2019 |
Verification Date | 2019-09-30 |
Last Update Posted Date | 2019-09-04 |
Facilities
Sequence: | 200390867 |
Name | Eugene Kim |
City | Daegu |
State | Nam-gu |
Zip | 42472 |
Country | Korea, Republic of |
Conditions
Sequence: | 52256822 | Sequence: | 52256823 | Sequence: | 52256824 | Sequence: | 52256825 | Sequence: | 52256826 |
Name | Anesthesia, General | Name | Electroencephalography | Name | Brain Waves | Name | Psychology, Children | Name | Child Behavior |
Downcase Name | anesthesia, general | Downcase Name | electroencephalography | Downcase Name | brain waves | Downcase Name | psychology, children | Downcase Name | child behavior |
Id Information
Sequence: | 40221009 |
Id Source | org_study_id |
Id Value | DCMC#7 |
Countries
Sequence: | 42636632 |
Name | Korea, Republic of |
Removed | False |
Design Outcomes
Sequence: | 177693373 | Sequence: | 177693367 | Sequence: | 177693368 | Sequence: | 177693369 | Sequence: | 177693370 | Sequence: | 177693371 | Sequence: | 177693372 | Sequence: | 177693374 | Sequence: | 177693375 |
Outcome Type | secondary | Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Delta-theta to alpha-beta ratio (DTABR) | Measure | Occurrence of Emergence delirium | Measure | Relative power of each brain waves | Measure | modified Yale preoperative anxiety score (mYPAS) | Measure | PAED score during PACU stay | Measure | FLACC score on initial, 10, 20, and 30 min | Measure | Watcha scale on initial, 10, 20, and 30 min | Measure | Delta to alpha ratio | Measure | Theta to beta ratio (TBR) |
Time Frame | From the cessation of sevoflurane inhalation to the extubation of airway devices such as tracheal tubes or laryngeal mask airway | Time Frame | During 60 minutes after PACU admission | Time Frame | From the cessation of sevoflurane inhalation to the extubation of airway devices such as tracheal tubes or laryngeal mask airway | Time Frame | before anesthesia induction (about 30 min before the surgery) | Time Frame | During 60 min after PACU admission | Time Frame | During 60 minutes after PACU admission] | Time Frame | During 60 minutes after PACU admission | Time Frame | From the cessation of sevoflurane inhalation to the extubation of airway devices such as tracheal tubes or laryngeal mask airway | Time Frame | From the cessation of sevoflurane inhalation to the extubation of airway devices such as tracheal tubes or laryngeal mask airway |
Description | From the relative power of each brain waves, the investigators calculated the ratio as follows:
DTABR = (Delta wave + Theta wave)/(alpha wave + beta wave) |
Description | On arrival at post-anesthesia care unit (PACU), patients are checked post-anesthesia emergence delirium (PAED). The PAED scale is a validated observational measure of 5 aspects of child behavior (caregiver eye contact, purposeful movement, evidence of awareness of surroundings, restlessness, and inconsolability). Ratings are summed to produce a total score ranging from 0 to 20; greater scores indicate greater severity.
If the PAED score is greater than 12, investigators define emergence delirium. |
Description | Original frontal EEG segments are attained via 2 channel bispectral index monitoring (BIS VISTA™, Aspect Medical Systems, Inc. MA, USA) during the anesthesia period. The EEG is then segmented into 4 s epochs and fast Fourier transform (FFT) analysis is performed for each of these segments. FFT of all these selected EEG segments are computed in the following frequency bands:
Delta: 1-4 Hz Theta: 4-8 Hz Alpha: 8-13 Hz Beta: 13-30 Hz And then, the relative power of each frequency bands to the total power of the sum is calculated. |
Description | mYPAS is the assessment tool for measure the anxiety before induction. Higher score indicates higher anxiety. | Description | On arrival at post-anesthesia care unit (PACU) and every 10 min from then, patients were checked PAED. The PAED scale is a validated observational measure of 5 aspects of child behavior (caregiver eye contact, purposeful movement, evidence of awareness of surroundings, restlessness, and inconsolability). Ratings are summed to produce a total score ranging from 0 to 20; greater scores indicate greater severity. | Description | Face, legs, activity, cry, and consolability (FLACC) score is checked every 10min after PACU admission | Description | On arrival and 10, 20, and 30 min after PACU admission, patients were checked Watcha scale as following 4-point scale
calm Higher score indicates higher agitation. |
Description | From the relative power of each brain waves, the investigators calculated the ratio as follows:
DAR = Delta wave / alpha wave |
Description | From the relative power of each brain waves, the investigators calculated the ratio as follows:
TBR = Theta wave / beta wave |
Sponsors
Sequence: | 48399390 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Daegu Catholic University Medical Center |
Overall Officials
Sequence: | 29331738 |
Role | Study Chair |
Name | Eugene Kim, MD, PhD |
Affiliation | Assistant professor |
Eligibilities
Sequence: | 30815169 |
Sampling Method | Non-Probability Sample |
Gender | All |
Minimum Age | 2 Years |
Maximum Age | 10 Years |
Healthy Volunteers | No |
Population | This study collects subjects from a tertiary university hospital. |
Criteria | Inclusion Criteria:
Children aged between 2 and 10 years of American Society of Anesthesiologists physical status (ASA PS) I or II who are planned to receive surgery under general anesthesia Exclusion Criteria: If the guardian and the subject are difficult to evaluate normally due to language barriers/language disorders/delay or autistic disorder |
Adult | False |
Child | True |
Older Adult | False |
Calculated Values
Sequence: | 254077172 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Actual Duration | 3 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 2 |
Maximum Age Num | 10 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 2 |
Number Of Secondary Outcomes To Measure | 7 |
Designs
Sequence: | 30561132 |
Observational Model | Cohort |
Time Perspective | Prospective |
Responsible Parties
Sequence: | 28927536 |
Responsible Party Type | Principal Investigator |
Name | Eugene Kim |
Title | Assistant professor |
Affiliation | Daegu Catholic University Medical Center |
Study References
Sequence: | 52155703 |
Pmid | 33010926 |
Reference Type | derived |
Citation | Kim J, Lee HC, Byun SH, Lim H, Lee M, Choung Y, Kim E. Frontal electroencephalogram activity during emergence from general anaesthesia in children with and without emergence delirium. Br J Anaesth. 2021 Jan;126(1):293-303. doi: 10.1016/j.bja.2020.07.060. Epub 2020 Oct 1. |
]]>
https://zephyrnet.com/NCT03797261
2019-03-18
https://zephyrnet.com/?p=NCT03797261
NCT03797261https://www.clinicaltrials.gov/study/NCT03797261?tab=tableNANANAThis dose-escalation study evaluating the safety, pharmacokinetics and preliminary efficacy of venetoclax in combination with AMG 176 in participants with relapsed or refractory acute myeloid leukemia (AML) and participants with Non-Hodgkin’s lymphoma (NHL)/diffuse large B-cell lymphoma (DLBCL).
This study will include a dose escalation phase to identify the maximum tolerated dose/recommended phase 2 dose (MTD/RPTD) of venetoclax plus AMG 176 as well as a dose expansion phase to confirm safety, explore efficacy, and confirm the suitability of the preliminary RPTD.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-07 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2021-12-07 |
Start Month Year | March 18, 2019 |
Primary Completion Month Year | December 30, 2019 |
Verification Month Year | December 2021 |
Verification Date | 2021-12-31 |
Last Update Posted Date | 2021-12-07 |
Facilities
Sequence: | 200754557 | Sequence: | 200754558 | Sequence: | 200754559 | Sequence: | 200754560 | Sequence: | 200754561 | Sequence: | 200754562 | Sequence: | 200754563 | Sequence: | 200754564 | Sequence: | 200754565 | Sequence: | 200754566 | Sequence: | 200754567 | Sequence: | 200754568 | Sequence: | 200754569 | Sequence: | 200754570 | Sequence: | 200754571 | Sequence: | 200754572 | Sequence: | 200754573 |
Name | City of Hope /ID# 207393 | Name | USC Norris Cancer Center /ID# 207396 | Name | University of Iowa Hospitals and Clinics /ID# 207459 | Name | Univ Kansas Med Ctr /ID# 207480 | Name | Duplicate_Dana-Farber Cancer Institute /ID# 207367 | Name | Washington University-School of Medicine /ID# 206995 | Name | NYU Langone Medical Center /ID# 207390 | Name | Unc /Id# 207388 | Name | UPMC Hillman Cancer Ctr /ID# 208482 | Name | Calvary Mater Newcastle /ID# 211455 | Name | Royal Adelaide Hospital /ID# 210602 | Name | Alfred Health /ID# 210350 | Name | Universitaetsklinikum Frankfurt /ID# 207984 | Name | Universitaetsklinikum Leipzig /ID# 209824 | Name | Charite Universitaetsklinikum Berlin – Campus Virchow /ID# 207987 | Name | Universitaetsklinikum Carl Gustav Carus an der TU Dresden /ID# 207803 | Name | Universitaetsklinikum Hamburg-Eppendorf (UKE) /ID# 207788 |
City | Duarte | City | Los Angeles | City | Iowa City | City | Kansas City | City | Boston | City | Saint Louis | City | New York | City | Chapel Hill | City | Pittsburgh | City | Waratah | City | Adelaide | City | Melbourne | City | Frankfurt am Main | City | Leipzig | City | Berlin | City | Dresden | City | Hamburg |
State | California | State | California | State | Iowa | State | Kansas | State | Massachusetts | State | Missouri | State | New York | State | North Carolina | State | Pennsylvania | State | New South Wales | State | South Australia | State | Victoria | State | Hessen | State | Sachsen | ||||||
Zip | 91010 | Zip | 90033 | Zip | 52242 | Zip | 66160 | Zip | 02215 | Zip | 63110 | Zip | 10016-6402 | Zip | 27599 | Zip | 15232 | Zip | 2298 | Zip | 5000 | Zip | 3004 | Zip | 60590 | Zip | 04103 | Zip | 13353 | Zip | 01307 | Zip | 20246 |
Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | United States | Country | Australia | Country | Australia | Country | Australia | Country | Germany | Country | Germany | Country | Germany | Country | Germany | Country | Germany |
Browse Interventions
Sequence: | 96346690 | Sequence: | 96346691 |
Mesh Term | Venetoclax | Mesh Term | Antineoplastic Agents |
Downcase Mesh Term | venetoclax | Downcase Mesh Term | antineoplastic agents |
Mesh Type | mesh-list | Mesh Type | mesh-ancestor |
Conditions
Sequence: | 52358496 | Sequence: | 52358497 | Sequence: | 52358498 |
Name | Acute Myeloid Leukemia | Name | Non-Hodgkin's Lymphoma | Name | Diffuse Large B-cell Lymphoma |
Downcase Name | acute myeloid leukemia | Downcase Name | non-hodgkin's lymphoma | Downcase Name | diffuse large b-cell lymphoma |
Id Information
Sequence: | 40292744 | Sequence: | 40292745 |
Id Source | org_study_id | Id Source | secondary_id |
Id Value | M16-785 | Id Value | 2018-003314-41 |
Id Type | EudraCT Number | ||
Countries
Sequence: | 42715852 | Sequence: | 42715853 | Sequence: | 42715854 |
Name | United States | Name | Australia | Name | Germany |
Removed | False | Removed | False | Removed | False |
Design Groups
Sequence: | 55801453 |
Group Type | Experimental |
Title | Venetoclax + AMG 176 |
Description | Venetoclax and AMG 176 will be administered in combination. Different combinations of dose levels for venetoclax and AMG 176 will be explored. |
Interventions
Sequence: | 52669438 | Sequence: | 52669439 |
Intervention Type | Drug | Intervention Type | Drug |
Name | Venetoclax | Name | AMG 176 |
Description | tablet, oral | Description | solution, intravenous |
Keywords
Sequence: | 80126133 | Sequence: | 80126134 | Sequence: | 80126135 | Sequence: | 80126136 | Sequence: | 80126137 | Sequence: | 80126138 |
Name | Acute Myeloid Leukemia | Name | Non-Hodgkin's Lymphoma | Name | Cancer | Name | Venetoclax | Name | AMG 176 | Name | diffuse large B-cell lymphoma (DLBCL) |
Downcase Name | acute myeloid leukemia | Downcase Name | non-hodgkin's lymphoma | Downcase Name | cancer | Downcase Name | venetoclax | Downcase Name | amg 176 | Downcase Name | diffuse large b-cell lymphoma (dlbcl) |
Design Outcomes
Sequence: | 178070364 | Sequence: | 178070365 | Sequence: | 178070366 | Sequence: | 178070367 | Sequence: | 178070368 | Sequence: | 178070369 | Sequence: | 178070370 | Sequence: | 178070371 | Sequence: | 178070372 | Sequence: | 178070373 | Sequence: | 178070374 | Sequence: | 178070375 |
Outcome Type | primary | Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Maximum Tolerated Dose (MTD) and/or Recommended Phase 2 Dose (RPTD) for Venetoclax + AMG 176 | Measure | Number of Participants With Adverse Events | Measure | Composite Complete Remission Rate (CRc) for Participants with AML | Measure | Objective Response Rate (ORR) for Participants with AML | Measure | ORR for Participants with NHL | Measure | Maximum Plasma Concentration (Cmax) of Venetoclax | Measure | Time to Maximum Observed Plasma Concentration (Tmax) of Venetoclax | Measure | AUC of Venetoclax | Measure | Maximum Plasma Concentration (Cmax) of AMG 176 | Measure | Half-life (t1/2) of AMG 176 | Measure | AUC of AMG 176 | Measure | Clearance (CL) of AMG 176 |
Time Frame | Up to 28 days after first dose of study drug in a dose-escalation phase | Time Frame | From first dose of study drug until 30 days or 5 half-lives after discontinuation of study drug administration will be collected (up to approximately 4 years). | Time Frame | Up to approximately 2 years from last subject first dose | Time Frame | Up to approximately 2 years from last subject first dose | Time Frame | Up to approximately 2 years from last subject first dose | Time Frame | Up to approximately 28 days after first dose of study drug | Time Frame | Up to approximately 28 days after first dose of study drug | Time Frame | Up to approximately 28 days after first dose of study drug | Time Frame | Up to approximately 16 days after first dose of study drug | Time Frame | Approximately 16 days after first dose of study drug | Time Frame | Approximately 16 days after first dose of study drug | Time Frame | Approximately 16 days after first dose of study drug |
Description | The MTD and/or RPTD of venetoclax and of AMG 176 will be determined during the dose escalation phase of the study. | Description | An adverse event (AE) is defined as any untoward medical occurrence in a patient or clinical investigation subject administered a pharmaceutical product and which does not necessarily have a causal relationship with this treatment. | Description | CRc rate is defined as CR + CRi (CR with incomplete blood count recovery). | Description | ORR is defined as the percentage of participants with documented partial response (PR) or better (CR + CRi + partial response [PR]) based on International Working Group (IWG) criteria for AML | Description | ORR is defined as the percentage of participants with documented CR + PR based on Lugano criteria for NHL. | Description | Maximum observed plasma concentration (Cmax) of venetoclax. | Description | Time to maximum plasma concentration (Tmax) of Venetoclax. | Description | Area under the plasma concentration-time curve (AUC) of venetoclax. | Description | Maximum observed plasma concentration (Cmax) of AMG 176 | Description | Terminal phase elimination half-life (t1/2) | Description | Area Under the Plasma Concentration-time Curve (AUC) of AMG 176 | Description | Clearance (CL) is defined the volume of plasma cleared of the drug per unit time. |
Browse Conditions
Sequence: | 194199540 | Sequence: | 194199541 | Sequence: | 194199542 | Sequence: | 194199543 | Sequence: | 194199544 | Sequence: | 194199545 | Sequence: | 194199546 | Sequence: | 194199547 | Sequence: | 194199548 | Sequence: | 194199549 | Sequence: | 194199550 | Sequence: | 194199551 | Sequence: | 194199552 | Sequence: | 194199553 | Sequence: | 194199554 | Sequence: | 194199555 |
Mesh Term | Lymphoma | Mesh Term | Leukemia, Myeloid | Mesh Term | Leukemia, Myeloid, Acute | Mesh Term | Lymphoma, Non-Hodgkin | Mesh Term | Lymphoma, B-Cell | Mesh Term | Lymphoma, Large B-Cell, Diffuse | Mesh Term | Hematologic Neoplasms | Mesh Term | Neoplasms by Histologic Type | Mesh Term | Neoplasms | Mesh Term | Lymphoproliferative Disorders | Mesh Term | Lymphatic Diseases | Mesh Term | Immunoproliferative Disorders | Mesh Term | Immune System Diseases | Mesh Term | Leukemia | Mesh Term | Neoplasms by Site | Mesh Term | Hematologic Diseases |
Downcase Mesh Term | lymphoma | Downcase Mesh Term | leukemia, myeloid | Downcase Mesh Term | leukemia, myeloid, acute | Downcase Mesh Term | lymphoma, non-hodgkin | Downcase Mesh Term | lymphoma, b-cell | Downcase Mesh Term | lymphoma, large b-cell, diffuse | Downcase Mesh Term | hematologic neoplasms | Downcase Mesh Term | neoplasms by histologic type | Downcase Mesh Term | neoplasms | Downcase Mesh Term | lymphoproliferative disorders | Downcase Mesh Term | lymphatic diseases | Downcase Mesh Term | immunoproliferative disorders | Downcase Mesh Term | immune system diseases | Downcase Mesh Term | leukemia | Downcase Mesh Term | neoplasms by site | Downcase Mesh Term | hematologic diseases |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48493518 | Sequence: | 48493519 | Sequence: | 48493520 |
Agency Class | INDUSTRY | Agency Class | INDUSTRY | Agency Class | INDUSTRY |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator |
Name | AbbVie | Name | Genentech, Inc. | Name | Amgen |
Overall Officials
Sequence: | 29384380 |
Role | Study Director |
Name | ABBVIE INC. |
Affiliation | AbbVie |
Design Group Interventions
Sequence: | 68404723 | Sequence: | 68404724 |
Design Group Id | 55801453 | Design Group Id | 55801453 |
Intervention Id | 52669438 | Intervention Id | 52669439 |
Eligibilities
Sequence: | 30873332 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Adequate kidney, liver and hematology values as described in the protocol. Exclusion Criteria: History of clinically significant medical condition that, in the opinion of the investigator, would adversely affect participation in this study. |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254045098 |
Number Of Facilities | 17 |
Registered In Calendar Year | 2019 |
Actual Duration | 9 |
Were Results Reported | False |
Has Us Facility | True |
Has Single Facility | False |
Minimum Age Num | 18 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 2 |
Number Of Secondary Outcomes To Measure | 10 |
Designs
Sequence: | 30619126 |
Allocation | N/A |
Intervention Model | Sequential Assignment |
Observational Model | |
Primary Purpose | Treatment |
Time Perspective | |
Masking | None (Open Label) |
Intervention Other Names
Sequence: | 26768509 |
Intervention Id | 52669438 |
Name | ABT-199 |
Links
Sequence: | 4402705 |
Url | http://www.rxabbvie.com |
Description | Related Info |
Responsible Parties
Sequence: | 28985653 |
Responsible Party Type | Sponsor |
]]>
https://zephyrnet.com/NCT03797248
2018-11-12
https://zephyrnet.com/?p=NCT03797248
NCT03797248https://www.clinicaltrials.gov/study/NCT03797248?tab=tableMing-Yen Tsai, PhDmissuriae@yahoo.com.tw+886975056534This 2-year trial is intended to be used to study breast cancer patients through forward-looking generation design through collaboration between Chinese and Western medical teams. The whole study consists of 2 stages, stage I comprises a cross-sectional study-baseline and stage II is a cohort for outcome evaluation and follow-up study across a 3-year period. To provide an empirical basis for combined TCM treatment in the Breast Cancer Research Team and to publish that as a reference for future TCM and Western medicine in integrative cancer treatment.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-05 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2019-09-17 |
Start Month Year | November 12, 2018 |
Primary Completion Month Year | October 24, 2020 |
Verification Month Year | September 2019 |
Verification Date | 2019-09-30 |
Last Update Posted Date | 2019-09-17 |
Detailed Descriptions
Sequence: | 20710014 |
Description | Breast cancer is a major health issue for women worldwide and has increased exponentially in the last decades. Improved earlier detection combined with adjuvant systemic therapy is responsible for much of the reduction in cause-specific mortality from breast cancer. Chemotherapy after surgery can decrease the risk of recurrence and is often used as routine treatment in clinic. Because of the fact that a considerable number of patients seek for traditional Chinese medicine (TCM) during adjuvant chemotherapy, it is thus need to evaluate the correlation between TCM treatment and prognosis. The investigators design a single center, prospective cohort study began in November 2018 in Kaohsiung, Taiwan. A sample of 104 participants diagnosed with early breast cancer was recruited from Breast Cancer Research Team and are followed up every 3 to 6 months till October 2023. Detailed information of participants includes general information, history of cancer, quality of life, side effects of chemotherapy and safety of treatment, body constitution of TCM and meridian energy analysis is taken face-to-face at baseline. |
Facilities
Sequence: | 199965204 |
Status | Recruiting |
Name | Kaohsiung Chang Gung Memorial Hospital |
City | Kaohsiung |
Zip | 83301 |
Country | Taiwan |
Facility Contacts
Sequence: | 28086689 |
Facility Id | 199965204 |
Contact Type | primary |
Name | Ming-Yen Tsai |
missuriae@yahoo.com.tw | |
Phone | +886975056534 |
Phone Extension | +886975056534 |
Conditions
Sequence: | 52139076 |
Name | Early-stage Breast Cancer |
Downcase Name | early-stage breast cancer |
Id Information
Sequence: | 40135115 |
Id Source | org_study_id |
Id Value | 201801559A3 |
Countries
Sequence: | 42542741 |
Name | Taiwan |
Removed | False |
Design Groups
Sequence: | 55559430 | Sequence: | 55559431 |
Title | Cohort 1 | Title | Cohort 2 |
Description | adjuvant chemotherapy combined with Chinese herbal medicine | Description | adjuvant chemotherapy only |
Interventions
Sequence: | 52454987 |
Intervention Type | Combination Product |
Name | Chinese herbal medicine |
Description | All Chinese herbal products prescribed from TCM physicians in our hospital during patients receiving adjuvant chemotherapy |
Keywords
Sequence: | 79822913 | Sequence: | 79822914 | Sequence: | 79822915 | Sequence: | 79822916 | Sequence: | 79822917 |
Name | traditional Chinese medicine | Name | quality of life | Name | disease-free survival | Name | adjuvant chemotherapy | Name | breast cancer |
Downcase Name | traditional chinese medicine | Downcase Name | quality of life | Downcase Name | disease-free survival | Downcase Name | adjuvant chemotherapy | Downcase Name | breast cancer |
Design Outcomes
Sequence: | 177264076 | Sequence: | 177264077 | Sequence: | 177264078 | Sequence: | 177264079 | Sequence: | 177264080 | Sequence: | 177264081 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | disease-free survival | Measure | QOLs measurement-1 | Measure | QOLs measurement-2 | Measure | TCM pattern | Measure | meridian energy | Measure | Side effects of adjuvant chemotherapy |
Time Frame | 3 years | Time Frame | 6 months | Time Frame | 6 months | Time Frame | 6 months | Time Frame | 6 months | Time Frame | 6 months |
Description | 3-year disease-free survival | Description | Functional Assessment of Cancer Therapy – Breast Cancer(FACT-B) | Description | Eastern Cooperative Oncology Group (ECOG) | Description | Body Constitution Questionnaire (BCQ) | Description | Meridian Energy Analysis Device (MEAD) | Description | Common Terminology Criteria for Adverse Events (CTCAE) |
Browse Conditions
Sequence: | 193366816 | Sequence: | 193366817 | Sequence: | 193366818 | Sequence: | 193366819 | Sequence: | 193366815 |
Mesh Term | Neoplasms by Site | Mesh Term | Neoplasms | Mesh Term | Breast Diseases | Mesh Term | Skin Diseases | Mesh Term | Breast Neoplasms |
Downcase Mesh Term | neoplasms by site | Downcase Mesh Term | neoplasms | Downcase Mesh Term | breast diseases | Downcase Mesh Term | skin diseases | Downcase Mesh Term | breast neoplasms |
Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-list |
Sponsors
Sequence: | 48290774 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Chang Gung Memorial Hospital |
Overall Officials
Sequence: | 29268565 |
Role | Principal Investigator |
Name | Chien-Ting Liu, MD |
Affiliation | Division of Oncology, Department of Internal Medicine |
Central Contacts
Sequence: | 12000505 |
Contact Type | primary |
Name | Ming-Yen Tsai, PhD |
Phone | +886975056534 |
missuriae@yahoo.com.tw | |
Role | Contact |
Design Group Interventions
Sequence: | 68107550 | Sequence: | 68107551 |
Design Group Id | 55559430 | Design Group Id | 55559431 |
Intervention Id | 52454987 | Intervention Id | 52454987 |
Eligibilities
Sequence: | 30747767 |
Sampling Method | Non-Probability Sample |
Gender | Female |
Minimum Age | 20 Years |
Maximum Age | N/A |
Healthy Volunteers | No |
Population | Patients with breast cancer aged over 20 years with histologically diagnosed stage 1-3 after radical surgery are enrolled from an academic medical center. All participants need to complete the 6-8 cycle of adjuvant chemotherapy, which may last 6 months. |
Criteria | Inclusion Criteria:
Aged > 20 years old female patients; Exclusion Criteria: Combined with inadequate heart, liver, kidney and hematopoietic function and other serious diseases; |
Adult | True |
Child | False |
Older Adult | True |
Calculated Values
Sequence: | 254122087 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 20 |
Minimum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 5 |
Designs
Sequence: | 30494050 |
Observational Model | Cohort |
Time Perspective | Prospective |
Responsible Parties
Sequence: | 28860330 |
Responsible Party Type | Principal Investigator |
Name | Ming-Yen Tsai |
Title | Department of Chinese medicine |
Affiliation | Chang Gung Memorial Hospital |
Study References
Sequence: | 52032796 |
Pmid | 31847861 |
Reference Type | derived |
Citation | Liu CT, Chen YH, Huang YC, Chen SY, Tsai MY. Chemotherapy in conjunction with traditional Chinese medicine for survival of patients with early female breast cancer: protocol for a non-randomized, single center prospective cohort study. Trials. 2019 Dec 17;20(1):741. doi: 10.1186/s13063-019-3848-8. |
]]>
https://zephyrnet.com/NCT03797235
2019-01-19
https://zephyrnet.com/?p=NCT03797235
NCT03797235https://www.clinicaltrials.gov/study/NCT03797235?tab=tableNANANAThe study aims to describe a correlation between the nerve cross section and the sensory or motor block onset time. Therefore, different nerve cross sections with their Motor and sensory onset times are compared in order to find a correlation.
In the case of discovering a correlation, this could be translated into clinical practice, where a more tailored and individualized approach to performing peripheral nerve blocks would be possible, thus lowering the risks of adverse events occurring.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-05 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2020-05-22 |
Start Month Year | January 19, 2019 |
Primary Completion Month Year | June 20, 2019 |
Verification Month Year | May 2020 |
Verification Date | 2020-05-31 |
Last Update Posted Date | 2020-05-22 |
Facilities
Sequence: | 200159508 |
Name | Der Balgrist |
City | Zürich |
Zip | 8008 |
Country | Switzerland |
Conditions
Sequence: | 52185583 |
Name | Regional Anesthesia |
Downcase Name | regional anesthesia |
Id Information
Sequence: | 40169132 |
Id Source | org_study_id |
Id Value | BASEC 2018-00939 |
Countries
Sequence: | 42580719 |
Name | Switzerland |
Removed | False |
Design Groups
Sequence: | 55609215 | Sequence: | 55609216 |
Group Type | Experimental | Group Type | Active Comparator |
Title | Dominant Arm | Title | Non-dominant arm |
Description | Two ultrasound guided nerve blocks (block of the ulnar and median nerve) on the dominant forearm | Description | Two ultrasound guided nerve blocks (block of the ulnar and median nerve) on the non-dominant forearm. |
Interventions
Sequence: | 52499517 | Sequence: | 52499518 |
Intervention Type | Procedure | Intervention Type | Procedure |
Name | Dominant Arm | Name | Non-dominant arm |
Description | The volume of local anesthetic used for the block of the ulnar and median nerve will be 5 times the estimated 95% effective dose (ED 95 ) of LA needed to block the nerve relative to the nerve cross-sectional area. The ED 95 for the ulnar nerve has been elucidated to be 0,11ml/mm2. The same ED 95 will be used for the median nerve. | Description | The volume of local anesthetic used for the block of the ulnar and median nerve will be 5 times the estimated 95% effective dose (ED 95 ) of LA needed to block the nerve relative to the nerve cross-sectional area. The ED 95 for the ulnar nerve has been elucidated to be 0,11ml/mm2. The same ED 95 will be used for the median nerve. |
Keywords
Sequence: | 79888898 |
Name | Ultrasound-guided regional anesthesia |
Downcase Name | ultrasound-guided regional anesthesia |
Design Outcomes
Sequence: | 177432337 | Sequence: | 177432338 | Sequence: | 177432339 | Sequence: | 177432340 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Correlation between nerve cross-section and time to complete sensory block of a nerve | Measure | Correlation between nerve cross-section and time to complete motor block of a nerve | Measure | Correlation between nerve cross-section and the duration of sensory nerve block | Measure | Correlation between the nerve cross-section and duration of motor nerve block |
Time Frame | Sensory evaluation will be carried out before the block and every 2 minutes after the start of the injection of LA until complete sensory loss to both cold and pinprick. Expected time frame: 10-60 minutes | Time Frame | Motor evaluation will be carried out before the block and every 2 minutes after the start of the injection of LA until complete motor block. Expected time frame: 10-100 minutes | Time Frame | The evaluation of the duration of block will start one hour after the determined complete sensory loss and will be tested every 10 minutes until complete resolution of the sensory block. Expected time frame: 10-300 minutes | Time Frame | The evaluation of the duration of sensory block will start one hour after the determined complete motor loss and will be tested every 10 minutes until complete resolution of the motor block. Expected time frame: 10-300min |
Description | Correlation between the nerve cross-section in mm2 of both nerves (median and ulnar) measured with an ultrasound system and time in minutes from the moment the investigator starts injecting the local anesthetic (LA) around the respective nerves to complete sensory loss in the innervation area of the blocked nerve, assessed by response to light touch, pinprick and cold sensation. This correlation will be expressed in min/ mm2. | Description | The correlation between the nerve cross-section area in mm2 of both nerves (median and ulnar) measured with an ultrasound system and time in minutes from the start of the LA injection around the nerve median and ulnar nerves to the respective onset of the motor block, assessed with a numerical scale ranging from 0 to 5 (0-no muscle contraction visible, 5-normal muscle strength, maximal force against resistance and gravity). This correlation will be expressed in min/ mm2. | Description | The correlation between the nerve cross-section area in mm2 of both nerves (median and ulnar) measured with an ultrasound system and the duration of the respective sensory block in minutes, as reflected by the return of normal sensation in the innervation area of the respective nerve. This correlation will be expressed in min/ mm2. | Description | The correlation between the nerve cross-section area in mm2 of both nerves (median and ulnar) measured with an ultrasound system and the duration of the respective motor block in minutes, as reflected by the return of normal muscle strength in the innervation area of the respective nerve. This correlation will be expressed in min/ mm2. |
Sponsors
Sequence: | 48332410 |
Agency Class | OTHER |
Lead Or Collaborator | lead |
Name | Jose Aguirre |
Overall Officials
Sequence: | 29293043 |
Role | Principal Investigator |
Name | José Aguirre, PD Dr Med |
Affiliation | Der Balgrist |
Design Group Interventions
Sequence: | 68168288 | Sequence: | 68168289 |
Design Group Id | 55609215 | Design Group Id | 55609216 |
Intervention Id | 52499517 | Intervention Id | 52499518 |
Eligibilities
Sequence: | 30773629 |
Gender | All |
Minimum Age | 18 Years |
Maximum Age | 64 Years |
Healthy Volunteers | Accepts Healthy Volunteers |
Criteria | Inclusion Criteria:
ASA I – II, both sexes Exclusion Criteria: Known allergy or hypersensitivity to a study drug or class of drug. |
Adult | True |
Child | False |
Older Adult | False |
Calculated Values
Sequence: | 253952969 |
Number Of Facilities | 1 |
Registered In Calendar Year | 2019 |
Actual Duration | 5 |
Were Results Reported | False |
Has Us Facility | False |
Has Single Facility | True |
Minimum Age Num | 18 |
Maximum Age Num | 64 |
Minimum Age Unit | Years |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 3 |
Designs
Sequence: | 30519760 |
Allocation | Randomized |
Intervention Model | Crossover Assignment |
Observational Model | |
Primary Purpose | Other |
Time Perspective | |
Masking | Single |
Subject Masked | True |
Responsible Parties
Sequence: | 28886061 |
Responsible Party Type | Sponsor-Investigator |
Name | Jose Aguirre |
Title | PD Dr. med. |
Affiliation | Balgrist University Hospital |
Study References
Sequence: | 52079059 | Sequence: | 52079060 | Sequence: | 52079061 | Sequence: | 52079062 | Sequence: | 52079063 | Sequence: | 52079064 | Sequence: | 52079065 | Sequence: | 52079066 | Sequence: | 52079067 | Sequence: | 52079068 | Sequence: | 52079069 | Sequence: | 52079070 | Sequence: | 52079071 | Sequence: | 52079072 |
Pmid | 19051446 | Pmid | 26361135 | Pmid | 19587623 | Pmid | 25644578 | Pmid | 25376973 | Pmid | 26423050 | Pmid | 14504153 | Pmid | 22664978 | Pmid | 20034967 | Pmid | 24809480 | Pmid | 21148659 | Pmid | 16857551 | Pmid | 2899106 | Pmid | 20121770 |
Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background | Reference Type | background |
Citation | Capdevila X, Biboulet P, Morau D, Mannion S, Choquet O. How and why to use ultrasound for regional blockade. Acta Anaesthesiol Belg. 2008;59(3):147-54. | Citation | Lewis SR, Price A, Walker KJ, McGrattan K, Smith AF. Ultrasound guidance for upper and lower limb blocks. Cochrane Database Syst Rev. 2015 Sep 11;2015(9):CD006459. doi: 10.1002/14651858.CD006459.pub3. | Citation | Eichenberger U, Stockli S, Marhofer P, Huber G, Willimann P, Kettner SC, Pleiner J, Curatolo M, Kapral S. Minimal local anesthetic volume for peripheral nerve block: a new ultrasound-guided, nerve dimension-based method. Reg Anesth Pain Med. 2009 May-Jun;34(3):242-6. doi: 10.1097/AAP.0b013e31819a7225. | Citation | Keplinger M, Marhofer P, Marhofer D, Schroegendorfer K, Haslik W, Zeitlinger M, Mayer CV, Kettner SC. Effective local anaesthetic volumes for sciatic nerve blockade: a clinical evaluation of the ED99. Anaesthesia. 2015 May;70(5):585-90. doi: 10.1111/anae.13013. Epub 2015 Jan 20. | Citation | Choi S, McCartney CJ. Evidence Base for the Use of Ultrasound for Upper Extremity Blocks: 2014 Update. Reg Anesth Pain Med. 2016 Mar-Apr;41(2):242-50. doi: 10.1097/AAP.0000000000000155. | Citation | Fenten MG, Schoenmakers KP, Heesterbeek PJ, Scheffer GJ, Stienstra R. Effect of local anesthetic concentration, dose and volume on the duration of single-injection ultrasound-guided axillary brachial plexus block with mepivacaine: a randomized controlled trial. BMC Anesthesiol. 2015 Sep 30;15:130. doi: 10.1186/s12871-015-0110-0. | Citation | Serradell A, Herrero R, Villanueva JA, Santos JA, Moncho JM, Masdeu J. Comparison of three different volumes of mepivacaine in axillary plexus block using multiple nerve stimulation. Br J Anaesth. 2003 Oct;91(4):519-24. doi: 10.1093/bja/aeg215. | Citation | Fredrickson MJ, Abeysekera A, White R. Randomized study of the effect of local anesthetic volume and concentration on the duration of peripheral nerve blockade. Reg Anesth Pain Med. 2012 Sep-Oct;37(5):495-501. doi: 10.1097/AAP.0b013e3182580fd0. | Citation | Latzke D, Marhofer P, Zeitlinger M, Machata A, Neumann F, Lackner E, Kettner SC. Minimal local anaesthetic volumes for sciatic nerve block: evaluation of ED 99 in volunteers. Br J Anaesth. 2010 Feb;104(2):239-44. doi: 10.1093/bja/aep368. Epub 2009 Dec 23. | Citation | Ecoffey C, Oger E, Marchand-Maillet F, Cimino Y, Rannou JJ, Beloeil H; SOS French Regional Anaesthesia Hotline. Complications associated with 27 031 ultrasound-guided axillary brachial plexus blocks: a web-based survey of 36 French centres. Eur J Anaesthesiol. 2014 Nov;31(11):606-10. doi: 10.1097/EJA.0000000000000063. | Citation | Jeng CL, Torrillo TM, Rosenblatt MA. Complications of peripheral nerve blocks. Br J Anaesth. 2010 Dec;105 Suppl 1:i97-107. doi: 10.1093/bja/aeq273. | Citation | Hebl JR. The importance and implications of aseptic techniques during regional anesthesia. Reg Anesth Pain Med. 2006 Jul-Aug;31(4):311-23. doi: 10.1016/j.rapm.2006.04.004. No abstract available. | Citation | Rotter ML, Hirschl AM, Koller W. Effect of chlorhexidine-containing detergent, non-medicated soap or isopropanol and the influence of neutralizer on bacterial pathogenicity. J Hosp Infect. 1988 Apr;11(3):220-5. doi: 10.1016/0195-6701(88)90100-4. | Citation | Marhofer P, Eichenberger U, Stockli S, Huber G, Kapral S, Curatolo M, Kettner S. Ultrasonographic guided axillary plexus blocks with low volumes of local anaesthetics: a crossover volunteer study. Anaesthesia. 2010 Mar;65(3):266-71. doi: 10.1111/j.1365-2044.2010.06247.x. Epub 2010 Jan 29. |
]]>
https://zephyrnet.com/NCT03797222
2019-04-15
https://zephyrnet.com/?p=NCT03797222
NCT03797222https://www.clinicaltrials.gov/study/NCT03797222?tab=tableNANANAInvestigators will assess the tolerability of oral Vitamin E supplementation in subjects with congenital hyperinsulinism (HI) and hyperammonemia (HA) syndrome.
<![CDATA[
Studies
Study First Submitted Date | 2019-01-06 |
Study First Posted Date | 2019-01-09 |
Last Update Posted Date | 2022-11-25 |
Start Month Year | April 15, 2019 |
Primary Completion Month Year | March 23, 2020 |
Verification Month Year | November 2022 |
Verification Date | 2022-11-30 |
Last Update Posted Date | 2022-11-25 |
Results First Posted Date | 2022-11-25 |
Detailed Descriptions
Sequence: | 20756417 |
Description | Congenital hyperinsulinism (HI) is a rare disorder of pancreatic beta cell insulin secretion that causes persistent and severe hypoglycemia starting at birth. Hyperinsulinism/hyperammonemia (HI/HA) syndrome is the second most common type of congenital HI and is caused by activating mutations in glutamate dehydrogenase (GDH). Patients with HI/HA exhibit fasting hyperinsulinemic hypoglycemia, protein-induced hypoglycemia, hyperammonemia, seizures, and intellectual disability independent of hypoglycemia. These effects result from abnormal GDH activity in the beta cells, liver and kidney cells, neurons, and astrocytes. The only available treatment for HI/HA syndrome is diazoxide, which acts on the beta cells to decrease insulin secretion but has no effect on GDH activity itself or on other cell types. Thus, there remains a significant unmet need for improved therapies for this disorder. Preliminary data show that Vitamin E (alpha-tocopherol) inhibits GDH activity in cell lines and improves hypoglycemia in a GDH HI mouse model. Based on these preclinical studies, Investigators hypothesize that Vitamin E will inhibit GDH activity and may impact hyperinsulinemic hypoglycemia and hyperammonemia in subjects with HI/HA syndrome. This hypothesis will be tested in a future study. In this initial pilot study, investigators will assess the tolerability of oral Vitamin E supplementation in subjects with HI/HA syndrome. |
Facilities
Sequence: | 200403436 |
Name | Children's Hospital of Philadelphia |
City | Philadelphia |
State | Pennsylvania |
Zip | 19104 |
Country | United States |
Browse Interventions
Sequence: | 96195107 | Sequence: | 96195105 | Sequence: | 96195106 | Sequence: | 96195108 | Sequence: | 96195109 | Sequence: | 96195110 | Sequence: | 96195111 | Sequence: | 96195112 | Sequence: | 96195113 |
Mesh Term | alpha-Tocopherol | Mesh Term | Vitamin E | Mesh Term | Tocopherols | Mesh Term | Vitamins | Mesh Term | Micronutrients | Mesh Term | Physiological Effects of Drugs | Mesh Term | Antioxidants | Mesh Term | Molecular Mechanisms of Pharmacological Action | Mesh Term | Protective Agents |
Downcase Mesh Term | alpha-tocopherol | Downcase Mesh Term | vitamin e | Downcase Mesh Term | tocopherols | Downcase Mesh Term | vitamins | Downcase Mesh Term | micronutrients | Downcase Mesh Term | physiological effects of drugs | Downcase Mesh Term | antioxidants | Downcase Mesh Term | molecular mechanisms of pharmacological action | Downcase Mesh Term | protective agents |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Conditions
Sequence: | 52260446 |
Name | Hyperinsulinism-Hyperammonemia Syndrome |
Downcase Name | hyperinsulinism-hyperammonemia syndrome |
Id Information
Sequence: | 40223701 | Sequence: | 40223702 |
Id Source | org_study_id | Id Source | secondary_id |
Id Value | 17-014550 | Id Value | T32DK063688 |
Id Type | U.S. NIH Grant/Contract | ||
Id Link | https://reporter.nih.gov/quickSearch/T32DK063688 |
Countries
Sequence: | 42639712 |
Name | United States |
Removed | False |
Design Groups
Sequence: | 55693336 |
Group Type | Experimental |
Title | Vitamin E Supplementation |
Description | Daily oral supplementation with Vitamin E (alpha-tocopherol) for 2 weeks. |
Interventions
Sequence: | 52573213 |
Intervention Type | Dietary Supplement |
Name | Vitamin E |
Description | Subjects will take an oral Vitamin E (alpha-tocopherol) supplement once daily with a fat-containing meal for 2 weeks. The dose will be based on subject age (150 IU if 1-3 years old, 300 IU if 4-8 years old, 450 IU if 9-17 years old, 600 IU if >17 years old). Formulations include 50 IU/mL liquid and 200 IU capsules. The liquid formulation will be used for subjects who will receive <600 IU daily, or for any subjects who prefer liquid medication to capsules. |
Keywords
Sequence: | 79995914 | Sequence: | 79995915 | Sequence: | 79995916 | Sequence: | 79995917 |
Name | hyperinsulinism | Name | hyperammonemia | Name | hypoglycemia | Name | vitamin e |
Downcase Name | hyperinsulinism | Downcase Name | hyperammonemia | Downcase Name | hypoglycemia | Downcase Name | vitamin e |
Design Outcomes
Sequence: | 177707526 | Sequence: | 177707527 | Sequence: | 177707528 | Sequence: | 177707529 | Sequence: | 177707530 | Sequence: | 177707531 | Sequence: | 177707532 | Sequence: | 177707533 | Sequence: | 177707534 | Sequence: | 177707535 | Sequence: | 177707536 |
Outcome Type | primary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary | Outcome Type | secondary |
Measure | Tolerability of Vitamin E Based on Responses to a Subject/Parent-reported Symptom Questionnaire After Vitamin E Supplementation Compared to Baseline | Measure | Plasma Alpha-tocopherol Concentration | Measure | Delta-plasma Glucose Concentration | Measure | Fasting Plasma Glucose Concentration | Measure | Nadir Plasma Glucose Concentration | Measure | Fasting Plasma Insulin Concentration | Measure | Peak Plasma Insulin Concentration | Measure | Delta-plasma Insulin Concentration | Measure | Fasting Plasma Ammonia Concentration | Measure | Delta-plasma Ammonia Concentration | Measure | Hypoglycemia Frequency |
Time Frame | 2 weeks | Time Frame | 2 weeks | Time Frame | 2 weeks | Time Frame | 2 weeks | Time Frame | 2 weeks | Time Frame | 2 weeks | Time Frame | 2 weeks | Time Frame | 2 weeks | Time Frame | 2 weeks | Time Frame | 2 weeks | Time Frame | 2 weeks |
Description | The following symptoms will be scored as either "none" (did not occur)=0, "mild" (minimal symptoms, no treatment needed)=1, "moderate" (symptoms requiring treatment at home or as an outpatient=2, or "severe" (symptoms requiring hospitalization or emergency room visit, or life-threatening or potentially life-threatening symptoms)=4:
Seizure, Headache, Vision change/blurred vision, Weakness, Fatigue, Nausea, Vomiting, Diarrhea, Stomach pain, Constipation, Bruising, Bleeding, Rash, Itching, Other Symptom scores will be summed to yield a Tolerability Questionnaire Score for each participant. The Tolerability Questionnaire Score has a minimum score of 0 (symptoms did not occur) and a maximum score of 60 (all of the measured symptoms occurred, each with severe designation). The number (count) of participants with an increase in Tolerability Questionnaire Score from baseline to 2 weeks (following Vitamin E supplementation) will be reported. |
Description | change in fasting plasma alpha-tocopherol concentration following Vitamin E supplementation (2 weeks [visit 2] – baseline [visit 1]) | Description | change in delta-glucose concentration (fasting plasma glucose – nadir plasma glucose during oral protein tolerance test) following Vitamin E supplementation (2 weeks [visit 2] – baseline [visit 1]) | Description | change in fasting plasma glucose concentration following Vitamin E supplementation (2 weeks [visit 2] – baseline [visit 1]) | Description | change in nadir plasma glucose concentration during oral protein tolerance test following Vitamin E supplementation (2 weeks [visit 2] – baseline [visit 1]) | Description | change in fasting plasma insulin concentration following Vitamin E supplementation (2 weeks [visit 2] – baseline [visit 1]) | Description | change in peak plasma insulin concentration during oral protein tolerance test following Vitamin E supplementation (2 weeks [visit 2] – baseline [visit 1]) | Description | change in delta-plasma insulin concentration (peak plasma insulin – fasting plasma insulin during oral protein tolerance test) following Vitamin E supplementation (2 weeks [visit 2] – baseline [visit 1]) | Description | change in fasting plasma ammonia concentration following Vitamin E supplementation (2 weeks [visit 2] – baseline [visit 1]) | Description | change in delta-plasma ammonia concentration (plasma ammonia at 60 minutes – fasting plasma ammonia during oral protein tolerance test) following Vitamin E supplementation (2 weeks [visit 2] – baseline [visit 1]) | Description | change in frequency of hypoglycemia (plasma glucose <70 mg/dL) detected on home glucose meter following Vitamin E supplementation (2 weeks [visit 2] – baseline [visit 1]) |
Browse Conditions
Sequence: | 193828218 | Sequence: | 193828219 | Sequence: | 193828220 | Sequence: | 193828221 | Sequence: | 193828222 | Sequence: | 193828223 | Sequence: | 193828224 |
Mesh Term | Hyperinsulinism | Mesh Term | Syndrome | Mesh Term | Hyperammonemia | Mesh Term | Disease | Mesh Term | Pathologic Processes | Mesh Term | Glucose Metabolism Disorders | Mesh Term | Metabolic Diseases |
Downcase Mesh Term | hyperinsulinism | Downcase Mesh Term | syndrome | Downcase Mesh Term | hyperammonemia | Downcase Mesh Term | disease | Downcase Mesh Term | pathologic processes | Downcase Mesh Term | glucose metabolism disorders | Downcase Mesh Term | metabolic diseases |
Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-list | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor | Mesh Type | mesh-ancestor |
Sponsors
Sequence: | 48402816 | Sequence: | 48402817 | Sequence: | 48402818 | Sequence: | 48402819 |
Agency Class | OTHER | Agency Class | OTHER | Agency Class | OTHER | Agency Class | NIH |
Lead Or Collaborator | lead | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator | Lead Or Collaborator | collaborator |
Name | Elizabeth A Rosenfeld | Name | University of Pennsylvania | Name | Lawson Wilkins Pediatric Endocrine Society | Name | National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) |
Overall Officials
Sequence: | 29333879 |
Role | Principal Investigator |
Name | Elizabeth Rosenfeld, MD |
Affiliation | Children's Hospital of Philadelphia |
Design Group Interventions
Sequence: | 68269834 |
Design Group Id | 55693336 |
Intervention Id | 52573213 |
Eligibilities
Sequence: | 30817373 |
Gender | All |
Minimum Age | 1 Year |
Maximum Age | 40 Years |
Healthy Volunteers | No |
Criteria | Inclusion Criteria:
Individuals age ≥12 months and ≤40 years Exclusion Criteria: Individuals age <12 months or >40 years |
Adult | True |
Child | True |
Older Adult | False |
Calculated Values
Sequence: | 254095062 |
Number Of Facilities | 1 |
Number Of Nsae Subjects | 34 |
Registered In Calendar Year | 2019 |
Actual Duration | 11 |
Were Results Reported | True |
Months To Report Results | 27 |
Has Us Facility | True |
Has Single Facility | True |
Minimum Age Num | 1 |
Maximum Age Num | 40 |
Minimum Age Unit | Year |
Maximum Age Unit | Years |
Number Of Primary Outcomes To Measure | 1 |
Number Of Secondary Outcomes To Measure | 10 |
Designs
Sequence: | 30563328 |
Allocation | N/A |
Intervention Model | Single Group Assignment |
Observational Model | |
Primary Purpose | Other |
Time Perspective | |
Masking | None (Open Label) |
Intervention Model Description | This open-label tolerability and feasibility pilot clinical study will use a before-and-after design, with blood tests and fasting oral protein tolerance test performed prior to and after 2 weeks of daily oral Vitamin E supplementation in individuals with HI/HA syndrome. |
Drop Withdrawals
Sequence: | 29040592 |
Result Group Id | 56158765 |
Ctgov Group Code | FG000 |
Period | Overall Study |
Reason | Withdrawal by Subject |
Count | 1 |
Intervention Other Names
Sequence: | 26715346 |
Intervention Id | 52573213 |
Name | alpha-tocopherol |
Milestones
Sequence: | 41077649 | Sequence: | 41077650 | Sequence: | 41077651 |
Result Group Id | 56158765 | Result Group Id | 56158765 | Result Group Id | 56158765 |
Ctgov Group Code | FG000 | Ctgov Group Code | FG000 | Ctgov Group Code | FG000 |
Title | STARTED | Title | COMPLETED | Title | NOT COMPLETED |
Period | Overall Study | Period | Overall Study | Period | Overall Study |
Count | 14 | Count | 13 | Count | 1 |
Participant Flows
Sequence: | 3926683 |
Outcome Counts
Sequence: | 74131006 | Sequence: | 74131007 | Sequence: | 74131008 | Sequence: | 74131009 | Sequence: | 74131010 | Sequence: | 74131011 | Sequence: | 74131012 | Sequence: | 74131013 | Sequence: | 74131014 | Sequence: | 74131015 | Sequence: | 74131016 |
Outcome Id | 30857536 | Outcome Id | 30857537 | Outcome Id | 30857538 | Outcome Id | 30857539 | Outcome Id | 30857540 | Outcome Id | 30857541 | Outcome Id | 30857542 | Outcome Id | 30857543 | Outcome Id | 30857544 | Outcome Id | 30857545 | Outcome Id | 30857546 |
Result Group Id | 56158766 | Result Group Id | 56158766 | Result Group Id | 56158766 | Result Group Id | 56158766 | Result Group Id | 56158766 | Result Group Id | 56158766 | Result Group Id | 56158766 | Result Group Id | 56158766 | Result Group Id | 56158766 | Result Group Id | 56158766 | Result Group Id | 56158766 |
Ctgov Group Code | OG000 | Ctgov Group Code | OG000 | Ctgov Group Code | OG000 | Ctgov Group Code | OG000 | Ctgov Group Code | OG000 | Ctgov Group Code | OG000 | Ctgov Group Code | OG000 | Ctgov Group Code | OG000 | Ctgov Group Code | OG000 | Ctgov Group Code | OG000 | Ctgov Group Code | OG000 |
Scope | Measure | Scope | Measure | Scope | Measure | Scope | Measure | Scope | Measure | Scope | Measure | Scope | Measure | Scope | Measure | Scope | Measure | Scope | Measure | Scope | Measure |
Units | Participants | Units | Participants | Units | Participants | Units | Participants | Units | Participants | Units | Participants | Units | Participants | Units | Participants | Units | Participants | Units | Participants | Units | Participants |
Count | 13 | Count | 12 | Count | 6 | Count | 12 | Count | 6 | Count | 12 | Count | 6 | Count | 6 | Count | 12 | Count | 5 | Count | 10 |
Provided Documents
Sequence: | 2588063 |
Document Type | Study Protocol and Statistical Analysis Plan |
Has Protocol | True |
Has Icf | False |
Has Sap | True |
Document Date | 2019-12-11 |
Url | https://ClinicalTrials.gov/ProvidedDocs/22/NCT03797222/Prot_SAP_000.pdf |
Reported Event Totals
Sequence: | 27986167 | Sequence: | 27986168 | Sequence: | 27986169 | Sequence: | 27986170 | Sequence: | 27986171 | Sequence: | 27986172 | Sequence: | 27986173 | Sequence: | 27986174 | Sequence: | 27986175 | Sequence: | 27986176 | Sequence: | 27986177 | Sequence: | 27986178 | Sequence: | 27986179 | Sequence: | 27986180 | Sequence: | 27986181 |
Ctgov Group Code | EG000 | Ctgov Group Code | EG000 | Ctgov Group Code | EG000 | Ctgov Group Code | EG001 | Ctgov Group Code | EG001 | Ctgov Group Code | EG001 | Ctgov Group Code | EG002 | Ctgov Group Code | EG002 | Ctgov Group Code | EG002 | Ctgov Group Code | EG003 | Ctgov Group Code | EG003 | Ctgov Group Code | EG003 | Ctgov Group Code | EG004 | Ctgov Group Code | EG004 | Ctgov Group Code | EG004 |
Event Type | serious | Event Type | other | Event Type | deaths | Event Type | serious | Event Type | other | Event Type | deaths | Event Type | serious | Event Type | other | Event Type | deaths | Event Type | serious | Event Type | other | Event Type | deaths | Event Type | serious | Event Type | other | Event Type | deaths |
Classification | Total, serious adverse events | Classification | Total, other adverse events | Classification | Total, all-cause mortality | Classification | Total, serious adverse events | Classification | Total, other adverse events | Classification | Total, all-cause mortality | Classification | Total, serious adverse events | Classification | Total, other adverse events | Classification | Total, all-cause mortality | Classification | Total, serious adverse events | Classification | Total, other adverse events | Classification | Total, all-cause mortality | Classification | Total, serious adverse events | Classification | Total, other adverse events | Classification | Total, all-cause mortality |
Subjects Affected | 0 | Subjects Affected | 9 | Subjects Affected | 0 | Subjects Affected | 0 | Subjects Affected | 1 | Subjects Affected | 0 | Subjects Affected | 0 | Subjects Affected | 2 | Subjects Affected | 0 | Subjects Affected | 0 | Subjects Affected | 3 | Subjects Affected | 0 | Subjects Affected | 0 | Subjects Affected | 3 | Subjects Affected | 0 |
Subjects At Risk | 14 | Subjects At Risk | 14 | Subjects At Risk | 14 | Subjects At Risk | 2 | Subjects At Risk | 2 | Subjects At Risk | 2 | Subjects At Risk | 5 | Subjects At Risk | 5 | Subjects At Risk | 5 | Subjects At Risk | 3 | Subjects At Risk | 3 | Subjects At Risk | 3 | Subjects At Risk | 4 | Subjects At Risk | 4 | Subjects At Risk | 4 |
Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 | Created At | 2023-08-09 15:19:48.411011 |
Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 | Updated At | 2023-08-09 15:19:48.411011 |
Reported Events
Sequence: | 529030973 | Sequence: | 529030974 | Sequence: | 529030975 | Sequence: | 529030976 | Sequence: | 529030977 | Sequence: | 529030978 | Sequence: | 529030979 | Sequence: | 529030971 | Sequence: | 529030972 | Sequence: | 529030963 | Sequence: | 529030964 | Sequence: | 529030965 | Sequence: | 529030966 | Sequence: | 529030967 | Sequence: | 529030968 | Sequence: | 529030969 | Sequence: | 529030970 | Sequence: | 529030980 | Sequence: | 529030981 | Sequence: | 529030982 | Sequence: | 529030983 | Sequence: | 529030984 | Sequence: | 529030985 | Sequence: | 529030986 | Sequence: | 529030987 | Sequence: | 529030988 | Sequence: | 529030989 | Sequence: | 529030990 | Sequence: | 529030991 | Sequence: | 529030992 | Sequence: | 529030993 | Sequence: | 529030994 | Sequence: | 529030995 | Sequence: | 529030996 | Sequence: | 529030997 | Sequence: | 529030998 | Sequence: | 529030999 | Sequence: | 529031000 | Sequence: | 529031001 | Sequence: | 529031002 |
Result Group Id | 56158767 | Result Group Id | 56158768 | Result Group Id | 56158769 | Result Group Id | 56158770 | Result Group Id | 56158771 | Result Group Id | 56158767 | Result Group Id | 56158768 | Result Group Id | 56158770 | Result Group Id | 56158771 | Result Group Id | 56158767 | Result Group Id | 56158768 | Result Group Id | 56158769 | Result Group Id | 56158770 | Result Group Id | 56158771 | Result Group Id | 56158767 | Result Group Id | 56158768 | Result Group Id | 56158769 | Result Group Id | 56158769 | Result Group Id | 56158770 | Result Group Id | 56158771 | Result Group Id | 56158767 | Result Group Id | 56158768 | Result Group Id | 56158769 | Result Group Id | 56158770 | Result Group Id | 56158771 | Result Group Id | 56158767 | Result Group Id | 56158768 | Result Group Id | 56158769 | Result Group Id | 56158770 | Result Group Id | 56158771 | Result Group Id | 56158767 | Result Group Id | 56158768 | Result Group Id | 56158769 | Result Group Id | 56158770 | Result Group Id | 56158771 | Result Group Id | 56158767 | Result Group Id | 56158768 | Result Group Id | 56158769 | Result Group Id | 56158770 | Result Group Id | 56158771 |
Ctgov Group Code | EG000 | Ctgov Group Code | EG001 | Ctgov Group Code | EG002 | Ctgov Group Code | EG003 | Ctgov Group Code | EG004 | Ctgov Group Code | EG000 | Ctgov Group Code | EG001 | Ctgov Group Code | EG003 | Ctgov Group Code | EG004 | Ctgov Group Code | EG000 | Ctgov Group Code | EG001 | Ctgov Group Code | EG002 | Ctgov Group Code | EG003 | Ctgov Group Code | EG004 | Ctgov Group Code | EG000 | Ctgov Group Code | EG001 | Ctgov Group Code | EG002 | Ctgov Group Code | EG002 | Ctgov Group Code | EG003 | Ctgov Group Code | EG004 | Ctgov Group Code | EG000 | Ctgov Group Code | EG001 | Ctgov Group Code | EG002 | Ctgov Group Code | EG003 | Ctgov Group Code | EG004 | Ctgov Group Code | EG000 | Ctgov Group Code | EG001 | Ctgov Group Code | EG002 | Ctgov Group Code | EG003 | Ctgov Group Code | EG004 | Ctgov Group Code | EG000 | Ctgov Group Code | EG001 | Ctgov Group Code | EG002 | Ctgov Group Code | EG003 | Ctgov Group Code | EG004 | Ctgov Group Code | EG000 | Ctgov Group Code | EG001 | Ctgov Group Code | EG002 | Ctgov Group Code | EG003 | Ctgov Group Code | EG004 |
Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. | Time Frame | Adverse event data were collected over the 2 week study period. |
Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other | Event Type | other |
Subjects Affected | 4 | Subjects Affected | 1 | Subjects Affected | 0 | Subjects Affected | 2 | Subjects Affected | 1 | Subjects Affected | 1 | Subjects Affected | 0 | Subjects Affected | 2 | Subjects Affected | 3 | Subjects Affected | 1 | Subjects Affected | 0 | Subjects Affected | 0 | Subjects Affected | 0 | Subjects Affected | 1 | Subjects Affected | 5 | Subjects Affected | 0 | Subjects Affected | 0 | Subjects Affected | 0 | Subjects Affected | 0 | Subjects Affected | 1 | Subjects Affected | 2 | Subjects Affected | 0 | Subjects Affected | 0 | Subjects Affected | 2 | Subjects Affected | 0 | Subjects Affected | 2 | Subjects Affected | 0 | Subjects Affected | 1 | Subjects Affected | 1 | Subjects Affected | 0 | Subjects Affected | 1 | Subjects Affected | 0 | Subjects Affected | 0 | Subjects Affected | 1 | Subjects Affected | 0 | Subjects Affected | 1 | Subjects Affected | 0 | Subjects Affected | 1 | Subjects Affected | 0 | Subjects Affected | 0 |
Subjects At Risk | 14 | Subjects At Risk | 2 | Subjects At Risk | 5 | Subjects At Risk | 3 | Subjects At Risk | 4 | Subjects At Risk | 14 | Subjects At Risk | 0 | Subjects At Risk | 3 | Subjects At Risk | 4 | Subjects At Risk | 14 | Subjects At Risk | 2 | Subjects At Risk | 5 | Subjects At Risk | 3 | Subjects At Risk | 4 | Subjects At Risk | 14 | Subjects At Risk | 2 | Subjects At Risk | 5 | Subjects At Risk | 0 | Subjects At Risk | 2 | Subjects At Risk | 3 | Subjects At Risk | 14 | Subjects At Risk | 2 | Subjects At Risk | 5 | Subjects At Risk | 3 | Subjects At Risk | 4 | Subjects At Risk | 14 | Subjects At Risk | 2 | Subjects At Risk | 5 | Subjects At Risk | 3 | Subjects At Risk | 4 | Subjects At Risk | 14 | Subjects At Risk | 2 | Subjects At Risk | 5 | Subjects At Risk | 3 | Subjects At Risk | 4 | Subjects At Risk | 14 | Subjects At Risk | 2 | Subjects At Risk | 5 | Subjects At Risk | 3 | Subjects At Risk | 4 |
Event Count | 6 | Event Count | 1 | Event Count | 0 | Event Count | 3 | Event Count | 2 | Event Count | 1 | Event Count | 0 | Event Count | 2 | Event Count | 4 | Event Count | 1 | Event Count | 0 | Event Count | 0 | Event Count | 0 | Event Count | 1 | Event Count | 6 | Event Count | 0 | Event Count | 0 | Event Count | 0 | Event Count | 0 | Event Count | 1 | Event Count | 2 | Event Count | 0 | Event Count | 0 | Event Count | 2 | Event Count | 0 | Event Count | 2 | Event Count | 0 | Event Count | 1 | Event Count | 1 | Event Count | 0 | Event Count | 1 | Event Count | 0 | Event Count | 0 | Event Count | 1 | Event Count | 0 | Event Count | 1 | Event Count | 0 | Event Count | 1 | Event Count | 0 | Event Count | 0 |
Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Reproductive system and breast disorders | Organ System | Reproductive system and breast disorders | Organ System | Nervous system disorders | Organ System | Nervous system disorders | Organ System | Infections and infestations | Organ System | Infections and infestations | Organ System | Infections and infestations | Organ System | Infections and infestations | Organ System | Infections and infestations | Organ System | Nervous system disorders | Organ System | Nervous system disorders | Organ System | Nervous system disorders | Organ System | Reproductive system and breast disorders | Organ System | Reproductive system and breast disorders | Organ System | Reproductive system and breast disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | Gastrointestinal disorders | Organ System | General disorders | Organ System | General disorders | Organ System | General disorders | Organ System | General disorders | Organ System | General disorders | Organ System | Skin and subcutaneous tissue disorders | Organ System | Skin and subcutaneous tissue disorders | Organ System | Skin and subcutaneous tissue disorders | Organ System | Skin and subcutaneous tissue disorders | Organ System | Skin and subcutaneous tissue disorders |
Adverse Event Term | Vomiting | Adverse Event Term | Vomiting | Adverse Event Term | Vomiting | Adverse Event Term | Vomiting | Adverse Event Term | Vomiting | Adverse Event Term | Increased menstrual bleeding | Adverse Event Term | Increased menstrual bleeding | Adverse Event Term | Headache | Adverse Event Term | Headache | Adverse Event Term | Otitis externa | Adverse Event Term | Otitis externa | Adverse Event Term | Otitis externa | Adverse Event Term | Otitis externa | Adverse Event Term | Otitis externa | Adverse Event Term | Headache | Adverse Event Term | Headache | Adverse Event Term | Headache | Adverse Event Term | Increased menstrual bleeding | Adverse Event Term | Increased menstrual bleeding | Adverse Event Term | Increased menstrual bleeding | Adverse Event Term | Abdominal pain | Adverse Event Term | Abdominal pain | Adverse Event Term | Abdominal pain | Adverse Event Term | Abdominal pain | Adverse Event Term | Abdominal pain | Adverse Event Term | Diarrhea | Adverse Event Term | Diarrhea | Adverse Event Term | Diarrhea | Adverse Event Term | Diarrhea | Adverse Event Term | Diarrhea | Adverse Event Term | Fatigue | Adverse Event Term | Fatigue | Adverse Event Term | Fatigue | Adverse Event Term | Fatigue | Adverse Event Term | Fatigue | Adverse Event Term | Rash | Adverse Event Term | Rash | Adverse Event Term | Rash | Adverse Event Term | Rash | Adverse Event Term | Rash |
Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 | Frequency Threshold | 0 |
Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment | Assessment | Systematic Assessment |
Responsible Parties
Sequence: | 28929725 |