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NCT00783692 Clinical Trial

Study of Vedolizumab (MLN0002) in Patients With Moderate to Severe Crohn's Disease

Crohn's Disease Clinical Trial

GEMINI II

Official title:
A Phase 3, Randomized, Placebo-Controlled, Blinded, Multicenter Study of the Induction and Maintenance of Clinical Response and Remission by Vedolizumab (MLN0002) in Patients With Moderate to Severe Crohn's Disease

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT00783692
Other study ID # C13007
Secondary ID 2008-002783-33U1
Status Completed
Phase Phase 3
First received October 31, 2008
Last updated June 19, 2014
Start date December 2008
Est. completion date May 2012

Study information
Verified date June 2014
Source Millennium Pharmaceuticals, Inc.
Contact n/a
Is FDA regulated No
Health authority United States: Food and Drug Administration
Study type Interventional

Clinical Trial Summary

The primary purpose of this study was to determine the effect of vedolizumab induction treatment on clinical response and remission at 6 weeks and to determine the effect of vedolizumab maintenance treatment on clinical remission at 52 weeks.

Description:

Study C13007 comprised 2 randomized, double-blind, placebo-controlled studies conducted under 1 protocol which, operationally, consisted of 2 phases.

- The Induction Phase, designed to establish the efficacy and safety of vedolizumab for the induction of clinical response and clinical remission, and

- The Maintenance Phase, designed to establish the efficacy and safety of vedolizumab for the maintenance of clinical response and clinical remission.

The 6-week Induction Phase contained 2 cohorts of participants: Cohort 1 participants were randomized and treated with double-blind study drug, and Cohort 2 participants were treated with open-label vedolizumab. The second cohort was enrolled to ensure that the sample size of Induction Phase responders randomized into the Maintenance Study provided sufficient power for the Maintenance Study primary efficacy analysis. These participants did not contribute to the efficacy analyses performed for the Induction Study. Participants in both cohorts were assessed for treatment response at Week 6.

In the Maintenance Phase vedolizumab-treated participants from both Cohort 1 and Cohort 2 who demonstrated a clinical response were randomized in a 1:1:1 ratio to double-blind treatment with vedolizumab administered every 4 weeks (Q4W), vedolizumab administered every 8 weeks (Q8W), or placebo. Vedolizumab-treated participants who did not demonstrate response at Week 6 continued treatment with open-label vedolizumab, administered Q4W. Participants treated with double-blind placebo in the Induction Phase continued on double-blind placebo during the Maintenance Phase, regardless of treatment response during induction. The Maintenance Phase began at Week 6 and concluded with Week 52 assessments.

After the Week 52 assessments, participants may have been eligible to enroll in Study C13008 (NCT00790933; Long-term Safety Study) to receive open-label vedolizumab treatment. Participants who withdrew early (prior to Week 52) due to sustained nonresponse, disease worsening, or the need for rescue medications may have been eligible to enroll in Study C13008. Participants who did not enroll into Study C13008 were to complete a final on-study safety assessment at Week 66 (or Final Safety visit 16 weeks after the last dose) in the Maintenance Phase of Study C13007.

Recruitment information / eligibility
Status Completed
Enrollment 1116
Est. completion date May 2012
Est. primary completion date March 2012
Accepts healthy volunteers No
Gender Both
Age group 18 Years to 80 Years
Eligibility Inclusion Criteria:

1. Age 18 to 80

2. Diagnosis of moderately to severely active Crohn's disease (CD)

3. CD involvement of the ileum and/or colon

4. Demonstrated, over the previous 5 year period, an inadequate response to, loss of response to, or intolerance of at least 1 of the following agents, within protocol-specified parameters:

1. Immunomodulators

2. Tumor necrosis factor-alpha (TNFa) antagonists

3. Corticosteroids

5. May be receiving a therapeutic dose of conventional therapies for irritable bowel disease (IBD) defined by the protocol

Exclusion Criteria

1. Evidence of abdominal abscess at the initial screening visit, other than a minimum of 10 aphthous ulcerations involving a minimum of 10 contiguous cm of intestine

2. Extensive colonic resection, subtotal or total colectomy

3. History of >3 small bowel resections or diagnosis of short bowel syndrome

4. Ileostomy, colostomy, or known fixed symptomatic stenosis of the intestine

5. Have received non permitted IBD therapies within either 30 or 60 days, depending on the medication, as stated in the protocol

6. Chronic hepatitis B or C infection

7. Active or latent tuberculosis

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Factorial Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment

Related Conditions & MeSH terms

Intervention

Drug:
vedolizumab
Vedolizumab for intravenous infusion
Other:
Placebo
Placebo intravenous infusion

Locations
Country Name City State
Canada GI Research Edmonton Alberta
Canada Zeidler Ledcor Center-Univerisity of Alberta Edmonton Alberta
Canada Royal University Hospital Saskatoon Saskatchewan
Puerto Rico Pharmaseek, LLC Ponce
United States Asheville Gastroenterology Associates, P.A. Asheville North Carolina
United States Atlanta Gastroenterology Associates Atlanta Georgia
United States University of Colorado Health Sciences Center Aurora Colorado
United States Austin Gastroenterology, PA Austin Texas
United States Gastroenterology Associates Baton Rouge Louisiana
United States Hepatobiliary Associates of New York Bayside New York
United States Northwest Gastroenterology Associates Bellevue Washington
United States Apex Clinical Trials Birmingham Alabama
United States University of Alabama at Birmingham Birmingham Alabama
United States Boston Medical Center Boston Massachusetts
United States Massachusetts General Hospital Boston Massachusetts
United States Connecticut Gastroenterology Institute Bristol Connecticut
United States University of North Carolina at Chapel Hill Chapel Hill North Carolina
United States Medical University Of SC CAR Charleston South Carolina
United States Charlotte Gastroentology and Hepatology, P.L.L.C Charlotte North Carolina
United States University of Virginia Health System Charlottesville Virginia
United States Digestive Health Physician Cheektowaga New York
United States Metropolitan Gastroenterology Group, P.C. Chevy Chase Maryland
United States Rush University Medical Center Chicago Illinois
United States University of Chicago Medical Center Chicago Illinois
United States Consultants for Clinical Research Inc. Cincinnati Ohio
United States Cleveland Clinic Foundation Cleveland Ohio
United States Digestive & Liver Consultants Clive Iowa
United States Iowa Digestive Disease Center Clive Iowa
United States Consultants in Gastroenterology Columbia South Carolina
United States Southeast Regional Research Group Columbus Georgia
United States Dayton Science Institute Dayton Ohio
United States The Center for Clinical Studies Dearborn Michigan
United States Atlanta Center for Gastroenterology, P.C. Decatur Georgia
United States Puget Sound Medical Research Edmonds Washington
United States Northwest Piedmont Clinical Research, Inc. Elkin North Carolina
United States Gastroenterology Associates of Northern Virginia Fairfax Virginia
United States University of Florida Gainesville Florida
United States Gastroenterology Center of the MidSouth, PC Germantown Tennessee
United States Rocky Mountain Clinical Research, LLC Golden Colorado
United States Long Island Clinical Research Associates Great Neck New York
United States Gastroenterology Center of Connecticut, P.C. Hamden Connecticut
United States Bayou City Research, Ltd. Houston Texas
United States Gastroenterology Consultants Houston Texas
United States Jacon Medical Research Associates Houston Texas
United States Indianapolis Gastroenterology & Hepatology, Inc.- ARC Indianapolis Indiana
United States Borland-Groover Clinic Jacksonville Florida
United States East Coast Institute for Research Jacksonville Florida
United States University of Florida, Jacksonville Jacksonville Florida
United States Truman Medical Center Kansas City Missouri
United States University Of Kansas Kansas City Kansas
United States Gastroenterology of the Rockies Lafayette Colorado
United States Dartmouth-Hitchcock Medical Center Lebanon New Hampshire
United States University of Kentucky Medical Center Lexington Kentucky
United States Arapahoe Gastroenterology Associates P.C. Littleton Colorado
United States South Denver Gastroenterology Lone Tree Colorado
United States Gastrointestinal Bioscience Los Angeles California
United States University Of Louisville Louisville Kentucky
United States Gastroenterology Associates of Central Georgia Macon Georgia
United States Pharmaseek, LLC Madison Wisconsin
United States Center for Advanced Gastroenterology Maitland Florida
United States Osler Clinical Research Melbourne Florida
United States Long Island Gastroenterology Group, P.C. Merrick New York
United States Center for Digestive and Liver Diseases, Inc. Mexico Missouri
United States University of Miami Miller School of Medicine Miami Florida
United States Medical College Of Wisconsin Milwaukee Wisconsin
United States Wisconsin Center for Advanced Research Milwaukee Wisconsin
United States Paramount Medical Specialty Montebello California
United States Burke Research Associates Morganton North Carolina
United States Affiliates in Gastroenterology PA Morristown New Jersey
United States Vanderbilt University Medical Center Nashville Tennessee
United States University of Medicine and Dentistry of New Jersey-NJMS New Brunswick New Jersey
United States United Medical Research Institute New Smyrna Beach Florida
United States New York Presbyterian Hospital New York New York
United States Present Chapman Marion Steinlauf MD PC New York New York
United States Digestive Research Associates Newnan Georgia
United States Digestive and Liver Disease Specialist Ltd. Norfolk Virginia
United States Compass Research LLC Orlando Florida
United States Internal Medicine Specialists Orlando Florida
United States Digestive Health Center Pasadena Texas
United States University of Pittsburgh Medical Center - Cancer Centers Pittsburgh Pennsylvania
United States Kim, Chung MD (Private Practice) Pittsford New York
United States Minnesota Gastroenterology, P.A. Plymouth Minnesota
United States The Oregon Clinic-West Hills Gastroenterology Portland Oregon
United States Shah Associates Prince Frederick Maryland
United States Lynn Institute of Pueblo Pueblo Colorado
United States Hunter Holmes McGuire VA Medical Center Richmond Virginia
United States Mayo Clinic Rochester Minnesota
United States University of Rochester Rochester New York
United States Capital Gastroenterology Consultants Medical Group Sacramento California
United States Alamo Medical Research San Antonio Texas
United States Gastroenterology Clinic of San Antonio San Antonio Texas
United States Stone Oak Research Foundation San Antonio Texas
United States Clinical Applications Laboratories Inc. San Diego California
United States Desta Digestive Disease Medical Center San Diego California
United States Granite Peaks Gastroenterology Sandy Utah
United States St. Joseph's/Candler Health System Savannah Georgia
United States Long Island Digestive Disease Consultants Setauket New York
United States DLW Research System Snellville Georgia
United States St. Louis Center for Clinical Research St. Louis Missouri
United States Washington University St. Louis Missouri
United States SUNY Stony Brook University Medical Center Stonybrook New York
United States Syracuse Gastroenterological Associates Syracuse New York
United States University of South Florida Tampa Florida
United States West Wind'r Research & Development, LLC Tampa Florida
United States Cotton O'Neil Digestive Health Center Topeka Kansas
United States Center for Digestive Health Troy Michigan
United States Options Health Research Tulsa Oklahoma
United States Digestive Health Specialists Tupelo Mississippi
United States Digestive Health Specialists of Tyler Tyler Texas
United States Carle Clinic Association P.C. Urbana Illinois
United States The Gastroenterology Group of South Jersey Vineland New Jersey
United States Wake Forest University Baptist Medical Center Winston Salem North Carolina
United States Shafran Gastroenterology Center Winter Park Florida
United States Gastroenterology Associates of Western Michigan, P.L.C. Wyoming Michigan

Sponsors (1)
Lead Sponsor Collaborator
Millennium Pharmaceuticals, Inc.

Countries where clinical trial is conducted

United States,  Canada,  Puerto Rico, 

Outcome
Type Measure Description Time frame Safety issue
Primary Induction Phase: Percentage of Participants Achieving Clinical Remission at Week 6 Clinical remission is defined as a Crohn's Disease Activity Index (CDAI) score = 150 points.
The CDAI is used to quantify the symptoms of patients with Crohn's disease and consists of eight factors, each summed after adjustment with a weighting factor. The components of the CDAI are:
Number of liquid or soft stools each day for 7 days;
Abdominal pain (graded from 0-3 on severity) each day for 7 days;
General well-being, subjectively assessed from 0 (well) to 4 (terrible) each day for 7 days;
Presence of complications;
Taking Lomotil or opiates for diarrhea;
Presence of an abdominal mass (0 as none, 2 as questionable, 5 as definite);
Hematocrit of < 0.47 in men and < 0.42 in women;
Percentage deviation from standard weight.
The total score ranges from 0 to approximately 600 and with higher scores indicating greater disease activity.
All participants who prematurely discontinued for any reason were considered as not achieving clinical remission.		 Week 6 No
Primary Induction Phase: Percentage of Participants With Enhanced Clinical Response at Week 6 Enhanced clinical response is defined as a CDAI score at least 100 points lower than Baseline. The CDAI is used to quantify the symptoms of patients with Crohn's disease and consists of eight factors, each summed after adjustment with a weighting factor. The components of the CDAI are:
Number of liquid or soft stools each day for 7 days;
Abdominal pain (graded from 0-3 on severity) each day for 7 days;
General well-being, subjectively assessed from 0 (well) to 4 (terrible) each day for 7 days;
Presence of complications;
Taking Lomotil or opiates for diarrhea;
Presence of an abdominal mass (0 as none, 2 as questionable, 5 as definite);
Hematocrit of < 0.47 in men and < 0.42 in women;
Percentage deviation from standard weight.
The total score ranges from 0 to 600 with higher scores indicating greater disease activity.
All participants who prematurely discontinued for any reason were considered as not achieving enhanced clinical response.		 Baseline and Week 6 No
Primary Maintenance Phase: Percentage of Participants Achieving Clinical Remission at Week 52 Clinical remission is defined as a CDAI score = 150. The CDAI is used to quantify the symptoms of patients with Crohn's disease and consists of eight factors, each summed after adjustment with a weighting factor. The components of the CDAI are:
Number of liquid or soft stools each day for 7 days;
Abdominal pain (graded from 0-3 on severity) each day for 7 days;
General well-being, subjectively assessed from 0 (well) to 4 (terrible) each day for 7 days;
Presence of complications;
Taking Lomotil or opiates for diarrhea;
Presence of an abdominal mass (0 as none, 2 as questionable, 5 as definite);
Hematocrit of < 0.47 in men and < 0.42 in women;
Percentage deviation from standard weight.
The total score ranges from 0 to 600 with higher scores indicating greater disease activity.
All participants who prematurely discontinued for any reason were considered as not achieving clinical remission.		 Week 52 No
Secondary Induction Phase: Change From Baseline in C-Reactive Protein (CRP) Levels at Week 6 C-reactive protein (CRP) is a protein found in the blood, the levels of which rise in response to inflammation. Normal concentration in healthy human serum is usually lower than 10 mg/L, slightly increasing with age. Higher levels indicate mild inflammation (10-40 mg/L) and active inflammation (40-200 mg/L). Baseline and Week 6 No
Secondary Maintenance Phase: Percentage of Participants With Enhanced Clinical Response at Week 52 Enhanced clinical response is defined as a CDAI score at least 100 points lower than the Baseline value. The CDAI is used to quantify the symptoms of patients with Crohn's disease and consists of eight factors, each summed after adjustment with a weighting factor. The components of the CDAI are:
Number of liquid or soft stools each day for 7 days;
Abdominal pain (graded from 0-3 on severity) each day for 7 days;
General well-being, subjectively assessed from 0 (well) to 4 (terrible) each day for 7 days;
Presence of complications;
Taking Lomotil or opiates for diarrhea;
Presence of an abdominal mass (0 as none, 2 as questionable, 5 as definite);
Hematocrit of < 0.47 in men and < 0.42 in women;
Percentage deviation from standard weight.
The total score ranges from 0 to 600 with higher scores indicating greater disease activity.
All participants who prematurely discontinued for any reason were considered as not achieving enhanced clinical response.		 Baseline and Week 52 No
Secondary Maintenance Phase: Percentage of Participants in Corticosteroid-free Clinical Remission at Week 52 Participants using oral corticosteroids at Baseline, who discontinued corticosteroids and were in clinical remission (CDAI score = 150) at Week 52 achieved corticosteroid-free clinical remission. The CDAI quantifies the symptoms of patients with Crohn's disease and consists of eight factors, summed after adjustment with a weighting factor. The total score ranges from 0 to 600 with higher scores indicating greater disease activity.
All participants who prematurely discontinued for any reason were considered as not achieving corticosteroid-free clinical remission.		 Week 52 No
Secondary Maintenance Phase: Percentage of Participants With Durable Clinical Remission Durable clinical remission is defined as CDAI score = 150 points at 80% or more of study visits during the Maintenance Phase, including the Week 52 visit (11 of 13 study visits). The CDAI quantifies the symptoms of patients with Crohn's disease and consists of eight factors, summed after adjustment with a weighting factor. The total score ranges from 0 to 600 with higher scores indicating greater disease activity.
All participants who prematurely discontinued for any reason were considered as not achieving durable clinical remission		 Assessed every 4 weeks from Week 6 to Week 50, and at Week 52 No
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