Colitis Ulcerative Clinical Trial
Official title:
A Phase 2, Multi-center, Randomized, Double-blind, Placebo-controlled Parallel-group Study to Evaluate the Efficacy and Safety of Dupilumab Therapy in Patients With Moderately to Severely Active Ulcerative Colitis With an Eosinophilic Phenotype
The protocol of this Phase 2 clinical trial consists of a double-blind, placebo-controlled, parallel-group, multicenter study to evaluate the efficacy and safety of dupilumab in participants with moderately to severely active Ulcerative Colitis (UC) with an eosinophilic phenotype. Screening period: 2 to up to 4 weeks Treatment period: 52-week investigational medicinal product (IMP) intervention (dupilumab or matching placebo) from Week 0 to Week 52 Open-label arm (optional): administration of open-label dupilumab therapy for study participants who qualify. Follow-up period: 12 weeks The maximum duration of study per participant is up to 68 weeks.
| Status | Recruiting |
| Enrollment | 84 |
| Est. completion date | February 20, 2026 |
| Est. primary completion date | May 16, 2025 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 18 Years and older |
| Eligibility | Inclusion Criteria: - Participants must be =18 years of age at the time of signing the informed consent. - Evidence of biomarker enrichment at time of screening. - Moderately to severely active UC, defined as a baseline modified Mayo score of 5 to 9, inclusive, using the Mayo endoscopic subscore assigned during the concurrent local and central reading of the video endoscopy. - Has a screening endoscopy with =2 endoscopic subscore in the Mayo score component assessment as determined by concurrent local and central reading of the video endoscopy. - Has a baseline rectal bleeding subscore of =1 and baseline a stool frequency score of =1 as determined by the Mayo score component assessment. - Participants with inadequate response/non-response, loss of response, or are intolerant of standard biologic therapy for their UC AND/OR Inadequate or non-responders, have shown loss of response, or are intolerant to at least 1 of the following treatments: oral corticosteroids (=20 mg/day), 5-aminosalicylic acid (ASA) compounds, immunomodulators, small molecules. Exclusion Criteria: Participants are excluded from the study if any of the following criteria apply: - Severe extensive colitis as evidenced by: - Current hospitalization - Likely to require surgery for the treatment of UC within 12 weeks of Screening Visit - UC limited to the rectum only or to <20 cm of the colon as determined by central reading. - Presence of an ileal pouch, ostomy, stoma or fistula or history of a fistula. - Require, or required within the 2 months before screening, surgery for active gastrointestinal bleeding, peritonitis, intestinal obstruction, or intra-abdominal or pancreatic abscess requiring surgical drainage, or other conditions possibly confounding the evaluation of benefit from study agent treatment. - Has a prior medical history of eosinophilic colitis. - Participants with abdominal abscess, fulminant disease, or toxic megacolon. - Participants with intestinal failure or short bowel syndrome. - Presence of symptomatic colonic or small bowel obstruction, confirmed by objective radiographic or endoscopic evidence of a stricture with resulting obstruction (dilation of the colon or small bowel proximal to the stricture on barium radiograph or an inability to traverse the stricture at endoscopy). - History of extensive colonic resection (eg, less than 30 cm of colon remaining) that would prevent adequate evaluation of the effect of study agent on clinical disease activity. - History of colonic mucosal dysplasia or presence of adenomatous colonic polyps not removed OR presence of colonic mucosal dysplasia or adenomatous colonic polyps not removed during colonoscopy at screening visit. - If the participant has extensive colitis for =8 years or disease limited to left side of colon (ie, distal to splenic flexure) for >10 years, regardless of age, a colonoscopy within 1 year of the screening visit is required to survey for dysplasia. Participants with dysplasia or cancer identified on biopsies will be excluded. - Diagnosis of indeterminate colitis, microscopic colitis, ischemic colitis, or Crohn's disease or clinical findings suggestive of Crohn's disease. The above information is not intended to contain all considerations relevant to a patient's potential participation in a clinical trial. |
| Country | Name | City | State |
|---|---|---|---|
| Argentina | Investigational Site Number : 0320002 | Caba | Ciudad De Buenos Aires |
| Argentina | Investigational Site Number : 0320006 | Mar del Plata | |
| Argentina | Investigational Site Number : 0320003 | Rosario | Santa Fe |
| Argentina | Investigational Site Number : 0320001 | San Miguel de Tucuman | |
| Argentina | Investigational Site Number : 0320004 | San Miguel de Tucumán | Tucumán |
| Canada | Investigational Site Number : 1240003 | Montreal | |
| Canada | Investigational Site Number : 1240006 | Montreal | Quebec |
| Chile | Investigational Site Number : 1520001 | Concepcion | Biobío |
| Chile | Investigational Site Number : 1520002 | Santiago | Reg Metropolitana De Santiago |
| Chile | Investigational Site Number : 1520003 | Santiago | Reg Metropolitana De Santiago |
| Chile | Investigational Site Number : 1520005 | Santiago | Reg Metropolitana De Santiago |
| Chile | Investigational Site Number : 1520006 | Santiago | |
| Japan | Investigational Site Number : 3920004 | Bunkyo-ku | Tokyo |
| Japan | Investigational Site Number : 3920011 | Kamakura-shi | |
| Japan | Investigational Site Number : 3920005 | Kashiwa-shi | |
| Japan | Investigational Site Number : 3920008 | Kitakyushu-shi | Fukuoka |
| Japan | Investigational Site Number : 3920007 | Kyoto-shi | Kyoto |
| Japan | Investigational Site Number : 3920006 | Nagoya-shi | Aichi |
| Japan | Investigational Site Number : 3920009 | Saitama-shi | |
| Japan | Investigational Site Number : 3920001 | Sapporo-shi | |
| Japan | Investigational Site Number : 3920002 | Sapporo-shi | |
| Japan | Investigational Site Number : 3920010 | Sunto-gun | Shizuoka |
| Korea, Republic of | Investigational Site Number : 4100003 | Busan | Busan-gwangyeoksi |
| Korea, Republic of | Investigational Site Number : 4100004 | Daegu | Daegu-gwangyeoksi |
| Korea, Republic of | Investigational Site Number : 4100005 | Daegu | |
| Korea, Republic of | Investigational Site Number : 4100006 | Daejeon | |
| Korea, Republic of | Investigational Site Number : 4100002 | Wonju | Gangwon-do |
| Mexico | Investigational Site Number : 4840004 | Cdmx | Ciudad De Mexico |
| Mexico | Investigational Site Number : 4840003 | Chihuahua | |
| Mexico | Investigational Site Number : 4840007 | Guadalajara | Jalisco |
| Mexico | Investigational Site Number : 4840005 | Saltillo | Coahuila De Zaragoza |
| Mexico | Investigational Site Number : 4840002 | Torreon | Coahuila De Zaragoza |
| Puerto Rico | Gastroenterology Research Unit, UPR Medical Sciences Campus Site Number : 6300002 | San Juan | |
| South Africa | Investigational Site Number : 7100002 | Cape Town | |
| South Africa | Investigational Site Number : 7100005 | Cape Town | |
| South Africa | Investigational Site Number : 7100007 | Cape Town | |
| South Africa | Investigational Site Number : 7100009 | Cape Town | |
| South Africa | Investigational Site Number : 7100001 | Johannesburg | |
| South Africa | Investigational Site Number : 7100006 | Johannesburg | |
| South Africa | Investigational Site Number : 7100008 | Kempton Park | |
| South Africa | Investigational Site Number : 7100003 | Port Elizabeth | |
| South Africa | Investigational Site Number : 7100004 | Pretoria | |
| Taiwan | Investigational Site Number : 1580002 | Taichung | |
| Turkey | Investigational Site Number : 7920002 | Ankara | |
| Turkey | Investigational Site Number : 7920003 | Gaziantep | |
| Turkey | Investigational Site Number : 7920005 | Istanbul | |
| Turkey | Investigational Site Number : 7920001 | Mersin | |
| Turkey | Investigational Site Number : 7920006 | Zonguldak | |
| United States | Om Research Site Number : 8400029 | Apple Valley | California |
| United States | Washington Gastroenterology Site Number : 8400025 | Bellevue | Washington |
| United States | Om Research Site Number : 8400028 | Camarillo | California |
| United States | Javara Research Site Number : 8400008 | Charlotte | North Carolina |
| United States | Gastro Center of Maryland Site Number : 8400021 | Columbia | Maryland |
| United States | Gastroenterology Associates, P.A. Site Number : 8400012 | Greenville | South Carolina |
| United States | Smart Medical Research Inc Site Number : 8400037 | Jackson Heights | New York |
| United States | Katy Integrative Gastroenterology Site Number : 8400027 | Katy | Texas |
| United States | TLC Clinical Research Inc Site Number : 8400020 | Los Angeles | California |
| United States | Care Access Research, Lumberton Site Number : 8400018 | Lumberton | North Carolina |
| United States | Gastroenterology Associates, PC Site Number : 8400032 | Manassas | Virginia |
| United States | Homestead Associates Site Number : 8400004 | Miami | Florida |
| United States | Wellness Clinical Research (WCR) Site Number : 8400009 | Miami Lakes | Florida |
| United States | Advanced Research Institute, Inc. Site Number : 8400026 | New Port Richey | Florida |
| United States | DiGiovanna Institute for Medical Education and Research Site Number : 8400006 | North Massapequa | New York |
| United States | Gastroenterology Consultants PC Site Number : 8400022 | Roswell | Georgia |
| United States | Medrasa Clinical Research Site Number : 8400039 | Sherman | Texas |
| United States | GI Alliance - Southlake Site Number : 8400013 | Southlake | Texas |
| United States | Washington Gastroenterology Site Number : 8400030 | Tacoma | Washington |
| United States | AdtreMed Site Number : 8400035 | Tampa | Florida |
| United States | GCP Clinical Research Site Number : 8400014 | Tampa | Florida |
| United States | Clinical Trials Management Service Site Number : 8400034 | Thousand Oaks | California |
| United States | Tyler Research Institute Site Number : 8400031 | Tyler | Texas |
| United States | Gastro Health & Nutrition Site Number : 8400019 | Victoria | Texas |
| Lead Sponsor | Collaborator |
|---|---|
| Sanofi | Regeneron Pharmaceuticals |
United States, Argentina, Canada, Chile, Japan, Korea, Republic of, Mexico, Puerto Rico, South Africa, Taiwan, Turkey,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Proportion of participants who are in clinical remission at Week 24 | Clinical remission by modified Mayo score is defined as a modified Mayo score of =2 with a stool frequency score =1, a rectal bleeding score = 0, AND a Mayo endoscopic subscore =1 with absence of friability. The modified Mayo score consists of 3 subscores; a patient-reported subscore for rectal bleeding, a patient-reported subscore for stool frequency, and a Mayo endoscopic subscore. Each subscore ranges 0-3 with higher scores indicating greater disease severity. The total modified Mayo score ranges 0-9 with higher scores indicating greater disease severity. | Week 24 | |
| Secondary | Proportion of participants achieving clinical response by modified Mayo score at Week 24 and Week 52 | Clinical response by modified Mayo score is defined as a decrease from baseline in the modified Mayo score of =2 points and at least a 30% reduction from baseline, and a decrease in rectal bleeding subscore of =1 OR an absolute rectal bleeding subscore of 0 or 1. The modified Mayo score consists of 3 subscores; a patient-reported subscore for rectal bleeding, a patient-reported subscore for stool frequency, and a Mayo endoscopic subscore. Each subscore ranges 0-3 with higher scores indicating greater disease severity. The total modified Mayo score ranges 0-9 with higher scores indicating greater disease severity. | Week 24 and Week 52 | |
| Secondary | Proportion of participants who are in clinical remission by modified Mayo score at Week 52 | Clinical remission by modified Mayo score is defined as a modified Mayo score of =2 with a stool frequency score =1, a rectal bleeding score = 0, AND a Mayo endoscopic subscore =1 with absence of friability. The modified Mayo score consists of 3 subscores; a patient-reported subscore for rectal bleeding, a patient-reported subscore for stool frequency, and a Mayo endoscopic subscore. Each subscore ranges 0-3 with higher scores indicating greater disease severity. The total modified Mayo score ranges 0-9 with higher scores indicating greater disease severity. | Week 52 | |
| Secondary | Proportion of participants in symptomatic remission over time | Symptomatic remission is defined as Mayo stool frequency score = 0, or Mayo stool frequency score = 1 with a =1-point decrease from baseline, and Mayo rectal bleeding score = 0. | Baseline up to Week 52 | |
| Secondary | Proportion of participants achieving histologic-endoscopic healing at Week 24, and Week 52 | Histologic-endoscopic healing is defined by Mayo endoscopic subscore of 0 or 1 and histological healing (Geboes score <2). Mayo endoscopic subscore ranges 0-3 with higher scores indicating greater disease severity. The Geboes Index score is a six-grade classification system for inflammation: Grade 0 - structural change only; Grade 1 -chronic inflammation; Grade 2 - lamina propria neutrophils; Grade 3 - neutrophils in epithelium; Grade 4 - crypt destruction; and Grade 5 - erosions or ulcers. | Week 24 and Week 52 | |
| Secondary | Proportion of participants with a Mayo endoscopic subscore of 0 or 1 without friability at Week 24, and Week 52 | The Mayo endoscopic subscore ranges 0-3 with higher scores indicating greater disease severity. | Week 24 and Week 52 | |
| Secondary | Proportion of participants with a Mayo endoscopic subscore of 0 at Week 24, and Week 52 | The Mayo endoscopic subscore ranges 0-3 with higher scores indicating greater disease severity. | Week 24 and Week 52 | |
| Secondary | Change from baseline in the partial Mayo score at Week 8, Week 24, and Week 52 | The partial Mayo score consists of 3 subscores; a patient-reported subscore for rectal bleeding, a patient-reported subscore for stool frequency, and a Physician's global assessment (PGA) subscore. Each subscore ranges 0-3 with higher scores indicating greater disease severity. The partial Mayo score ranges 0-9 with higher scores indicating greater disease severity. | Baseline to Week 8, Week 24 and Week 52 | |
| Secondary | Proportion of participants in clinical remission at Week 52 who are off concomitant oral corticosteroids (OCS) at least 4 weeks prior to Week 52 | Clinical remission by modified Mayo score is defined as a modified Mayo score of =2 with a stool frequency score =1, a rectal bleeding score = 0, AND a Mayo endoscopic subscore =1 with absence of friability. The modified Mayo score consists of 3 subscores; a patient-reported subscore for rectal bleeding, a patient-reported subscore for stool frequency, and a Mayo endoscopic subscore. Each subscore ranges 0-3 with higher scores indicating greater disease severity. The total modified Mayo score ranges 0-9 with higher scores indicating greater disease severity. | Baseline up to Week 52 | |
| Secondary | Proportion of participants in clinical remission at Week 52 who are off concomitant oral corticosteroids (OCS) at least 4 weeks prior to Week 52 among participants receiving OCS at baseline | Clinical remission by modified Mayo score is defined as a modified Mayo score of =2 with a stool frequency score =1, a rectal bleeding score = 0, AND a Mayo endoscopic subscore =1 with absence of friability. The modified Mayo score consists of 3 subscores; a patient-reported subscore for rectal bleeding, a patient-reported subscore for stool frequency, and a Mayo endoscopic subscore. Each subscore ranges 0-3 with higher scores indicating greater disease severity. The total modified Mayo score ranges 0-9 with higher scores indicating greater disease severity. | Baseline up to Week 52 | |
| Secondary | Change from baseline in abdominal pain assessed by Abdominal Pain Numerical Rating Scale (NRS) at Week 8, Week 24, and Week 52 | Abdominal pain NRS is a single item patient report outcome (PRO) tool that patients will use to report intensity of their worst abdominal pain during a daily recall period with 0 being 'no pain' and 10 being the 'worst pain imaginable'. | Baseline to Week 8, Week 24 and Week 52 | |
| Secondary | Incidence of treatment-emergent adverse events (TEAEs) or serious adverse events (SAEs) | Baseline up to Week 64 | ||
| Secondary | Concentration of dupilumab in serum over time. | Baseline up to Week 64 | ||
| Secondary | Incidence of treatment-emergent antidrug antibodies (ADA) against dupilumab. | Baseline up to Week 64 | ||
| Secondary | Change from baseline (Screening visit) in the normalized enrichment scores (NES) in type 2 inflammation transcriptome signature at Week 24 and Week 52. | NES is a summary score of the expression of a specified set of genes defining a molecular phenotype. | Baseline to Week 24 and Week 52 |
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Recruiting |
NCT05588843 -
Dose-finding Study of SAR443122 in Adult Participants With Ulcerative Colitis
|
Phase 2 | |
| Completed |
NCT01331551 -
Mesalamine and Reproductive Health Study
|