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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT01696396
Other study ID # 20110232
Secondary ID 2012-000529-31
Status Completed
Phase Phase 2
First received
Last updated
Start date December 4, 2012
Est. completion date April 10, 2018

Study information

Verified date May 2019
Source Amgen
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The primary objective of this study is to evaluate the efficacy of abrilumab as measured by the proportion of participants achieving Crohn's Disease Activity Index (CDAI) remission (CDAI < 150) after treatment for 8 weeks.


Description:

The study consisted of a 24-week double-blind treatment period, a 108-week open-label treatment period, and a 2-year safety follow-up period.

Participants who did not reach minimal improvement, or experienced disease worsening after initial response, had the option to receive open-label abrilumab 210 mg every 3 months (Q3M) beginning at double-blind period week 12 or after. Not reaching minimal improvement was defined as not having an improvement in CDAI score of ≥ 70 points from baseline on 2 consecutive visits (at or after week 8) at least 2 weeks apart. Disease worsening after week 8 (or week 12) response was defined as having an increase in CDAI score of ≥ 70 points from the week 8 (or week 12) CDAI score on 2 consecutive visits at least 2 weeks apart, and a CDAI score of > 150.

Participants were planned to be randomized in a 2:1:2:1 ratio to SC placebo or abrilumab at 21 mg, 70 mg (on day 1, week 2, week 4, and every 4 weeks thereafter until week 24), or 210 mg (on day 1 followed by placebo in weeks 2 and 4 and every 4 weeks thereafter until week 24), respectively. Due to a consistent discrepancy between the investigational product (IP) instruction manual (IPIM) description of vial positions and the actual vial positions in the IP package participants were initially randomized to 3 arms (placebo, 70 mg, and 210 mg) with a randomization ratio of 3:2:1. The study was temporarily paused while this issue was investigated. Once the discrepancy was corrected, Protocol Amendment 3 implemented, and affected participants completed their double-blind treatment period, the study resumed enrollment and randomization per protocol. Neither the randomization nor study blind was compromised and therefore the intent-to-treat principle was maintained.


Recruitment information / eligibility

Status Completed
Enrollment 254
Est. completion date April 10, 2018
Est. primary completion date December 26, 2014
Accepts healthy volunteers No
Gender All
Age group 18 Years to 65 Years
Eligibility Inclusion Criteria:

- Diagnosed with ileal, ileo-colonic, or colonic Crohn's disease for a minimum of 6 months prior to baseline

- Moderately to severely active Crohn's disease defined by a CDAI score = 220 and = 450 at baseline

- Evidence of active inflammation within 12 weeks prior to baseline

- Demonstrated an inadequate response to, loss of response to, or intolerance to at least one of the following agents: Immunomodulators and/or anti-tumor necrosis factor (TNF) agents or to corticosteroids (non-US sites only).

- Neurological exam free of clinically significant, unexplained signs or symptoms during screening and no clinically significant change prior to randomization

- Subject has no known history of active tuberculosis and has a negative test for tuberculosis during screening

Exclusion Criteria:

- Short bowel syndrome

- Stricture with obstructive symptoms within 3 months

- Bowel surgery within 12 weeks prior baseline, or has planned bowel surgery within 24 weeks from baseline

- Ileostomy and/or colostomy

- Any gastric or intestinal pouch

- Evidence of an infected abscess

- Bowel perforation or evidence of non-inflammatory obstruction during the 6 months prior to baseline

- Stool positive for C. difficile toxin at screening

- Any uncontrolled or clinically significant systemic disease

- Known to have tested positive for hepatitis B virus surface antigen, hepatitis C virus antibody, or human immunodeficiency virus (HIV)

- Any underlying condition that predisposes subject to infections

- Subject has malignancy (other than resected cutaneous basal or cutaneous squamous cell carcinoma, or treated in situ cervical cancer considered cured) within 5 years of baseline

- Received an anti-TNF agent, cyclosporine, mycophenolate mofetil, sirolimus (rapamycin), thalidomide, tacrolimus, topical (rectal) aminosalicylic acid (eg, mesalamine) or topical (rectal) steroids, intravenous or intramuscular corticosteroids within protocol-specified time periods.

- Any prior exposure to antagonists of integrins or integrin ligands (eg, natalizumab, efalizumab, or vedolizumab), rituximab, or TNF kinoid immunotherapies, AMG 181, or any form of cell-based transplantation

- Received treatment of infection with intravenous (within 30 days of baseline) or oral (within 14 days prior to baseline) antibiotics, antivirals, or antifungals

- Significant laboratory abnormalities

- Pregnant or breast feeding

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Abrilumab
Administered by subcutaneous injection.
Placebo
Placebo matching to abrilumab administered by subcutaneous injection

Locations

Country Name City State
Austria Research Site Innsbruck
Austria Research Site St Veit an der Glan
Austria Research Site Wien
Austria Research Site Wien
Belgium Research Site Bonheiden
Belgium Research Site Brussels
Belgium Research Site Gent
Belgium Research Site Leuven
Canada Research Site Edmonton Alberta
Canada Research Site London Ontario
Canada Research Site Saskatoon Saskatchewan
Canada Research Site Sudbury Ontario
Canada Research Site Toronto Ontario
Canada Research Site Vancouver British Columbia
Canada Research Site Winnipeg Manitoba
Czechia Research Site Hradec Kralove
Czechia Research Site Praha 4
Czechia Research Site Praha 4
Czechia Research Site Praha 5
Czechia Research Site Praha 7
Czechia Research Site Usti nad Labem
Denmark Research Site Aalborg
Denmark Research Site Århus C
Denmark Research Site Herlev
Denmark Research Site Hvidovre
Denmark Research Site Køge
Denmark Research Site Odense C
France Research Site Amiens Cedex 1
France Research Site Caen Cedex 9
France Research Site Clichy
France Research Site Lille
France Research Site Nice Cedex 3
France Research Site Paris Cedex 10
France Research Site Paris cedex 12
France Research Site Pessac Cedex
France Research Site Vandoeuvre les Nancy
Germany Research Site Hamburg
Germany Research Site Leipzig
Germany Research Site Minden
Germany Research Site Stuttgart
Hungary Research Site Bekescsaba
Hungary Research Site Budapest
Hungary Research Site Budapest
Hungary Research Site Debrecen
Hungary Research Site Miskolc
Hungary Research Site Szekszard
Netherlands Research Site Amsterdam
Netherlands Research Site Breda
Netherlands Research Site Leiden
Netherlands Research Site Maastricht
Netherlands Research Site Rotterdam
Switzerland Research Site Basel
Switzerland Research Site Bern
Switzerland Research Site Zurich
United Kingdom Research Site Birmingham
United Kingdom Research Site Coventry
United Kingdom Research Site London
United Kingdom Research Site Manchester
United Kingdom Research Site Norwich
United Kingdom Research Site Torquay
United States Research Site Ann Arbor Michigan
United States Research Site Arlington Heights Illinois
United States Research Site Atlanta Georgia
United States Research Site Birmingham Alabama
United States Research Site Charlotte North Carolina
United States Research Site Chesterfield Michigan
United States Research Site Dothan Alabama
United States Research Site Germantown Tennessee
United States Research Site Goodyear Arizona
United States Research Site Great Neck New York
United States Research Site Greenville North Carolina
United States Research Site Jacksonville Florida
United States Research Site La Jolla California
United States Research Site Mentor Ohio
United States Research Site Mexico Missouri
United States Research Site Mobile Alabama
United States Hospital New York New York
United States Research Site New York New York
United States Research Site Oklahoma City Oklahoma
United States Research Site Philadelphia Pennsylvania
United States Research Site Phoenix Arizona
United States Research Site Rochester Minnesota
United States Research Site Sanford Florida
United States Research Site Seattle Washington

Sponsors (1)

Lead Sponsor Collaborator
Amgen

Countries where clinical trial is conducted

United States,  Austria,  Belgium,  Canada,  Czechia,  Denmark,  France,  Germany,  Hungary,  Netherlands,  Switzerland,  United Kingdom, 

References & Publications (1)

Dummer R, Hoeller C, Gruter IP, Michielin O. Combining talimogene laherparepvec with immunotherapies in melanoma and other solid tumors. Cancer Immunol Immunother. 2017 Jun;66(6):683-695. doi: 10.1007/s00262-017-1967-1. Epub 2017 Feb 25. Review. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary Percentage of Participants With Remission at Week 8 Remission was defined as a Crohn's Disease Activity Index (CDAI) score < 150 at week 8.
The CDAI is a weighted, composite index of 8 disease variables (stool frequency, severity of abdominal pain, degree of general well-being, presence or absence of extra-intestinal manifestations or fistula, use or non-use of antidiarrheal agents, presence or absence of an abdominal mass, hematocrit, and body weight). Scores range from approximately 0 to 600, with a higher score indicating more-severe disease activity.
The remission rate (percentage of participants with remission) was calculated based on observed data (unadjusted remission rate) and also after applying a logistic regression model including the factors of treatment group, stratification factors (prior anti-TNF use and pre- versus post-Protocol Amendment 3) and baseline CDAI Score (adjusted remission rate).
Week 8
Secondary Percentage of Participants With Remission at Week 12 Remission was defined as a Crohn's Disease Activity Index (CDAI) score < 150. The CDAI is a weighted, composite index of 8 disease variables (stool frequency, severity of abdominal pain, degree of general well-being, presence or absence of extra-intestinal manifestations or fistula, use or non-use of antidiarrheal agents, presence or absence of an abdominal mass, hematocrit, and body weight). Scores range from approximately 0 to 600, with a higher score indicating more-severe disease activity.
The remission rate (percentage of participants with remission) was calculated based on observed data (unadjusted remission rate) and also after applying a logistic regression model including the factors of treatment group, stratification factors (prior anti-TNF use and pre- versus post-Protocol Amendment 3) and baseline CDAI Score (adjusted remission rate).
Week 12
Secondary Percentage of Participants With Response at Week 12 Response was defined as either remission (a CDAI score < 150) or a decrease from baseline in the CDAI score of = 100 points.
The CDAI is a weighted, composite index of 8 disease variables (stool frequency, severity of abdominal pain, degree of general well-being, presence or absence of extra-intestinal manifestations or fistula, use or non-use of antidiarrheal agents, presence or absence of an abdominal mass, hematocrit, and body weight). Scores range from approximately 0 to 600, with a higher score indicating more-severe disease activity.
The response rate (percentage of participants with response) was calculated based on observed data (unadjusted response rate) and also after applying a logistic regression model including the factors of treatment group, stratification factors (prior anti-TNF use and pre- versus post-Protocol Amendment 3) and baseline CDAI score (adjusted response rate).
Baseline and week 12
Secondary Percentage of Participants With Response at Week 8 Response was defined as either remission (a CDAI score < 150) or a decrease from baseline in the CDAI score of = 100 points.
The CDAI is a weighted, composite index of 8 disease variables (stool frequency, severity of abdominal pain, degree of general well-being, presence or absence of extra-intestinal manifestations or fistula, use or non-use of antidiarrheal agents, presence or absence of an abdominal mass, hematocrit, and body weight). Scores range from approximately 0 to 600, with a higher score indicating more-severe disease activity.
The response rate (percentage of participants with response) was calculated based on observed data (unadjusted response rate) and also after applying a logistic regression model including the factors of treatment group, stratification factors (prior anti-TNF use and pre- versus post-Protocol Amendment 3) and baseline CDAI score (adjusted response rate).
Baseline and week 8
Secondary Percentage of Participants With Sustained Remission at Both Week 12 and Week 24 Remission was defined as a Crohn's Disease Activity Index (CDAI) score < 150. Sustained remission was defined as achieving the criteria for remission at both week 12 and week 24.
The CDAI is a weighted, composite index of 8 disease variables (stool frequency, severity of abdominal pain, degree of general well-being, presence or absence of extra-intestinal manifestations or fistula, use or non-use of antidiarrheal agents, presence or absence of an abdominal mass, hematocrit, and body weight). Scores range from approximately 0 to 600, with a higher score indicating more-severe disease activity.
The remission rate (percentage of participants with sustained remission) was calculated based on observed data (unadjusted remission rate) and also after applying a logistic regression model including the factors of treatment group, stratification factors (prior anti-TNF use and pre- versus post-Protocol Amendment 3) and baseline CDAI Score (adjusted remission rate).
Week 12 and week 24
Secondary Percentage of Participants With Sustained Remission at Both Week 8 and Week 24 Remission was defined as a Crohn's Disease Activity Index (CDAI) score < 150. Sustained remission was defined as achieving the criteria for remission at both week 8 and week 24.
The CDAI is a weighted, composite index of 8 disease variables (stool frequency, severity of abdominal pain, degree of general well-being, presence or absence of extra-intestinal manifestations or fistula, use or non-use of antidiarrheal agents, presence or absence of an abdominal mass, hematocrit, and body weight). Scores range from approximately 0 to 600, with a higher score indicating more-severe disease activity.
The remission rate (percentage of participants with sustained remission) was calculated based on observed data (unadjusted remission rate) and also after applying a logistic regression model including the factors of treatment group, stratification factors (prior anti-TNF use and pre- versus post-Protocol Amendment 3) and baseline CDAI Score (adjusted remission rate).
Week 8 and week 24
Secondary Change From Baseline in CDAI Score at Week 12 The CDAI is a weighted, composite index of 8 disease variables (stool frequency, severity of abdominal pain, degree of general well-being, presence or absence of extra-intestinal manifestations or fistula, use or non-use of antidiarrheal agents, presence or absence of an abdominal mass, hematocrit, and body weight). Scores range from approximately 0 to 600, with a higher score indicating more-severe disease activity. Baseline and week 12
Secondary Change From Baseline in CDAI Score at Week 8 The CDAI is a weighted, composite index of 8 disease variables (stool frequency, severity of abdominal pain, degree of general well-being, presence or absence of extra-intestinal manifestations or fistula, use or non-use of antidiarrheal agents, presence or absence of an abdominal mass, hematocrit, and body weight). Scores range from approximately 0 to 600, with a higher score indicating more-severe disease activity. Baseline and week 8
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