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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02871635
Other study ID # 1297.4
Secondary ID 2016-000612-14
Status Completed
Phase Phase 3
First received
Last updated
Start date September 28, 2016
Est. completion date May 13, 2019

Study information

Verified date May 2020
Source Boehringer Ingelheim
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Primary Objective:

The primary objective of this trial is to compare the clinical efficacy of BI 695501 with EU-approved Humira® in patients with active Crohn's disease (CD).

Secondary Objectives:

The secondary objectives of this trial are to compare the efficacy and safety of BI 695501 with EU-approved Humira® across the induction and maintenance phases.


Recruitment information / eligibility

Status Completed
Enrollment 147
Est. completion date May 13, 2019
Est. primary completion date April 30, 2019
Accepts healthy volunteers No
Gender All
Age group 18 Years to 80 Years
Eligibility Inclusion criteria:

- Males and females aged >=18 and =<80 years at Screening who have a diagnosis of moderate to severely active Crohn's Disease (CD), confirmed by endoscopy or radiologic evaluation, for more than 4 months with evidence of mucosal ulceration. Patients must have all of the following:

- Crohn's Disease Activity Index (CDAI) score of >=220 and =<450

- A diagnosis of Crohn's Disease (CD) confirmed by ileocolonoscopy during Screening

- Presence of mucosal ulcers in at least one segment of the ileum or colon and a SES-CD score =7 (for patients with isolated ileal disease SES-CD score =4), as assessed by ileocolonoscopy and confirmed by central independent reviewer(s) before randomization

- Anti-tumor necrosis factor (TNF) patients or patients previously treated with infliximab who had initially responded and who meet one of the following criteria:

- Responded and developed secondary resistance due confirmed anti-infliximab anti-drug antibody formation, which caused infliximab depletion

- Responded and became intolerant

- Further inclusion criteria apply

Exclusion criteria:

- Patients with ulcerative colitis or indeterminate colitis

- Patients with symptomatic known obstructive strictures

- Surgical bowel resection performed within 6 months prior to Screening or planned resection at any time while enrolled in the trial

- Patients with an ostomy or ileoanal pouch

- Patients with short bowel syndrome

- Patients who have previously used infliximab and have never clinically responded

- Patients who have previously received treatment with adalimumab, or who have participated in an adalimumab or adalimumab biosimilar clinical trial

- Further exclusion criteria apply

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
BI 695501

HUMIRA


Locations

Country Name City State
Belarus Gomel Regional Clinical Gomel
Belarus City Clinical Hospital # 10 Minsk
Belarus Vitebsk Regional Clinical Oncology Dispensary Vitebsk
Bosnia and Herzegovina University Clinical Centre Sarajevo Sarajevo
Croatia Clinical Hospital Osijek Osijek
Croatia Polyclinic Bonifarm Zagreb
Czechia Vojenska nemocnice Brno Brno
Czechia Hepato-Gastroenterologie HK, s.r.o. Hradec Kralove
Czechia CTCenter Mave, s.r.o., Cllinical Trials Center, Olomouc Olomouc
Czechia Gregar s.r.o. Olomouc
Czechia PreventaMed, s.r.o. Olomouc
Czechia University Hospital Ostrava Ostrava-Poruba
Czechia Vitkovice Hospital Ostrava-Vitkovice
Czechia Medicon, a.s. Prague
Czechia Axon Clinical, s.r.o. Praha
Czechia University Hospital Na Bulovce Praha 8
Czechia General Hospital Pribram Pribram
Czechia Masaryk Hospital, Internal Department Usti nad Labem
Germany Crohn Colitis Centrum Rhein Main Frankfurt
Greece General Hospital of Athens Evangelismos Athens
Greece University General Hospital of Heraklion Heraklion, Crete
Greece General Hospital of Rhodes Rhodes
Israel Haemek Medical Center Afula
Israel Wolfson Medical Center Holon
Israel Hadassah Medical Center, Ein-Karem Jerusalem
Israel Meir Medical Center Kfar-Saba
Israel The Chaim Sheba Medical Center Tel Hashomer Ramat Gan
Israel Kaplan Medical Center Rehovot
Poland KLIMED Marek Klimkiewicz Bialystok
Poland NZOZ Centrum Medyczne KERmed Bydgoszcz
Poland Medical Center Pleiades Cracow
Poland Polimedica Centrum Badan Kielce
Poland Indywidualna Specjalistyczna Praktyka Lekarska Maciej Zymla Knurow
Poland SANTA FAMILIA Centrum Badan, Profilaktyki i Leczenia Lodz
Poland Clinic Medical Center; Nowa Sol Nowa Sol
Poland Ai Medical Center, private practice, Poznan Poznan
Poland Gabinet Lekarski Bartosz Korczowski Rzeszow
Poland Specialized Medical Practice. Dr med. Marek Horynski Sopot
Poland Twoja Przychodnia-Szczecinskie Centrum Medyczne Szczecin
Russian Federation Multidisciplinary Medical Clinic "Anthurium" Barnaul
Russian Federation GUZ Reg. Clinical Hospital, Kemerovo Kemerovo
Russian Federation Clinical Hospital No. 24, Moscow Moscow
Russian Federation Murmansk Regional Clinical Hospital named after Bayandin Murmansk
Russian Federation Reg.Clin.Hosp.n.a.Semashko Nizhniy Novgorod
Russian Federation FSBSI "Scientific and Research Institute of Physiology and Basic Medicine" Novosibirsk
Russian Federation State Novosibirsk Regional Clinical Hospital Novosibirsk
Russian Federation BHI of Omsk region - Clinical Oncology Dispensary Omsk
Russian Federation LLC IClinic Saint Petersburg
Russian Federation SBIH City Clinical Hospital #31 Saint Petersburg
Russian Federation NonState Healthcare Institution Central Clinical Hospital, Samara station JSC "Russian Railways" Samara
Russian Federation Private Educational Institution of Higher Education "Medical University "REAVIZ" Samara
Russian Federation Baltic Med,LLC Clinic BaltMed Ozerki St. Petersburg
Russian Federation EKO-Bezopasnost, St. Petersburg St. Petersburg
Serbia Clinical Center Bezanijska kosa, Belgrade Belgrade
Serbia Clinical Center Zemun Belgrade
Serbia Clinical Medical Center Zvezdara, Belgrade Belgrade
Serbia Military Medical Academy Belgrade
Serbia Clinical Center Kragujevac Kragujevac
Turkey Gazi University Medical Faculty Ankara
Turkey Gaziantep University Medical Faculty Sahinbey Educational Research Hospital Gaziantep
Turkey Kartal Lutfi Kirdar Research and Training Hospital Istanbul
Turkey Kocaeli University Research and Training Hospital Kocaeli
Ukraine CI Cherkasy RH of Cherkasy Reg.Council Cherkasy
Ukraine CHI Prof.O.O.Shalimov Kharkiv City Clinical Hospital #2 Kharkiv
Ukraine Med Center 'Ok!Clinic+' of International Institute of Clinical Trials LLC Kiev
Ukraine Private Enterprise Private Manufacturing Company "Acinus" Kirovohrad
Ukraine Clin Hosp.8 P.L.Shupyk NMA of PGE Kyiv
Ukraine Medical Center Medical Clinic Kyiv Kyiv
Ukraine M.I. Pyrogov VRCH, Vinnytsia Vinnytsia
Ukraine Vinnytsia M.I. Pyrogov NMU Ch of internal medicine #3 Vinnytsia
Ukraine Clin.Hosp#1,Zaporizhzhia Zaporizhzhia
United Kingdom Royal Bournemouth and Christchurch Hospital Bournemouth
United Kingdom Walsall Manor Hospital Walsall
United States Asheville Gastroenterology Associates, PA Asheville North Carolina
United States MGG Group Co. Inc. / Chevy Chase Clinical Research, Chevy Chase Maryland
United States Gastro Center of Maryland Columbia Maryland
United States Doctors Clinical Research East Point Georgia
United States Gastroenterology Associates, PA Greenville South Carolina
United States Healthcare Research Network Hazelwood Missouri
United States Houston Endoscopy and Research Center Houston Texas
United States Borland-Groover Clinic Jacksonville Florida
United States University of Kansas Medical Center Kansas City Kansas
United States Biopharma Informatic, Inc, dba Research Consultants Katy Texas
United States Hope Clinical Research Kissimmee Florida
United States Center for Advanced GI Maitland Florida
United States Great Lakes Gastroenterology Research, LLC Mentor Ohio
United States Advance Medical Research Center Miami Florida
United States Advanced Research Institute, Inc New Port Richey Florida
United States Southwest Gastroenterology Oak Lawn Illinois
United States Sagact, Pllc San Antonio Texas
United States Baylor Scott and White Healthcare Temple Texas
United States Victoria Gastroenterology Victoria Texas

Sponsors (1)

Lead Sponsor Collaborator
Boehringer Ingelheim

Countries where clinical trial is conducted

United States,  Belarus,  Bosnia and Herzegovina,  Croatia,  Czechia,  Germany,  Greece,  Israel,  Poland,  Russian Federation,  Serbia,  Turkey,  Ukraine,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Percentage of Patients With a Clinical Response (CDAI Decrease of =70 Compared With Baseline) at Week 4 The Crohn's Disease Activity Index (CDAI) is a validated instrument to measure disease severity in Crohn's Disease (CD). The CDAI score is a sum of the 8 factors (number of liquid stools, abdominal pain, general well-being, extra-intestinal complications, antidiarrheal drugs, abdominal mass, hematocrit and body weight) after adjustment with a weighting factor. Higher CDAI scores indicating more active disease.
The CDAI decrease at Week 4 was assessed as the decrease relative to baseline measurement, patients with a decrease =70 were responders.
Percentage=least squares means per treatment group back transformed using inverse logit function. Missing data were imputed according to non-responder imputation (NRI) and last observation carried forward (LOCF).
Week 4
Secondary Percentage of Patients With a Clinical Response (CDAI Decrease of =70 Compared With Baseline) at Week 24 The CDAI is a validated instrument to measure disease severity in CD. The CDAI score is a sum of the 8 factors (number of liquid stools, abdominal pain, general well-being, extra-intestinal complications, antidiarrheal drugs, abdominal mass, hematocrit and body weight) after adjustment with a weighting factor. Higher CDAI scores indicating more active disease.
The CDAI decrease at Week 24 was assessed as the decrease relative to baseline measurement, patients with a decrease =70 were responders.
Percentage=least squares means per treatment group back transformed using inverse logit function. Missing data were imputed according to NRI and LOCF.
Week 24
Secondary Percentage of Patients in Clinical Remission (CDAI <150) at Week 24 The CDAI is a validated instrument to measure disease severity in CD. The CDAI score is a sum of the 8 factors (number of liquid stools, abdominal pain, general well-being, extra-intestinal complications, antidiarrheal drugs, abdominal mass, hematocrit and body weight) after adjustment with a weighting factor. Higher CDAI scores indicating more active disease.
Patients with CDAI <150 at Week 24 were considered as clinical remission cases. Percentage=least squares means per treatment group back transformed using inverse logit function. Missing data were imputed according to NRI and LOCF.
at Week 24
Secondary Percentage of Patients With Adverse Events (AEs), Serious AEs (SAEs), and AEs of Special Interest (AESIs) Analysis of AEs focused on treatment-emergent AEs (TEAEs). For the period 1 'Baseline - Week 24', TEAEs were defined as AEs that started or worsened on or after first dose of trial medication and prior to date of the Week 24 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients who discontinued treatment before Week 24. For the period 2 'Week 24 - Week 46', TEAEs were defined as AEs that started or worsened on Week 24 visit and prior to or on Week 56 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients discontinuing treatment prior to Week 46. TEAEs and SAEs (including investigator-assessed trial medication-related TEAEs) and AESIs are reported. The following were considered an AESI: hepatic injury, anaphylactic reactions, serious infection and hypersensitivity reactions. From first administration of trial medication until 10 weeks after last administration, up to a maximum of 56 weeks.
Secondary Percentage of Patients With Infections The percentage of patients with TEAEs for infections are reported. For the period 1 'Baseline - Week 24', TEAEs were defined as AEs that started or worsened on or after first dose of trial medication and prior to date of the Week 24 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients who discontinued treatment before Week 24. For the period 2 'Week 24 - Week 46', TEAEs were defined as AEs that started or worsened on Week 24 visit and prior to or on Week 56 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients discontinuing treatment prior to Week 46. From first administration of trial medication until 10 weeks after last administration, up to a maximum of 56 weeks.
Secondary Percentage of Patients With Serious Infections The percentage of patients with TEAEs for serious infections are reported. For the period 1 'Baseline - Week 24', TEAEs were defined as AEs that started or worsened on or after first dose of trial medication and prior to date of the Week 24 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients who discontinued treatment before Week 24. For the period 2 'Week 24 - Week 46', TEAEs were defined as AEs that started or worsened on Week 24 visit and prior to or on Week 56 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients discontinuing treatment prior to Week 46. From first administration of trial medication until 10 weeks after last administration, up to a maximum of 56 weeks.
Secondary Percentage of Patients Who Experienced Hypersensitivity Reactions The percentage of patients with TEAEs for hypersensitivity reactions is reported. For the period 1 'Baseline - Week 24', TEAEs were defined as AEs that started or worsened on or after first dose of trial medication and prior to date of the Week 24 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients who discontinued treatment before Week 24. For the period 2 'Week 24 - Week 46', TEAEs were defined as AEs that started or worsened on Week 24 visit and prior to or on Week 56 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients discontinuing treatment prior to Week 46. From first administration of trial medication until 10 weeks after last administration, up to a maximum of 56 weeks.
Secondary Percentage of Patients Who Experienced Drug Induced Liver Injury (DILI) The percentage of patients with TEAEs for DILIs is reported. For the period 1 'Baseline - Week 24', TEAEs were defined as AEs that started or worsened on or after first dose of trial medication and prior to date of the Week 24 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients who discontinued treatment before Week 24. For the period 2 'Week 24 - Week 46', TEAEs were defined as AEs that started or worsened on Week 24 visit and prior to or on Week 56 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients discontinuing treatment prior to Week 46. From first administration of trial medication until 10 weeks after last administration, up to a maximum of 56 weeks.
Secondary Percentage of Patients With Injection Site Reactions The percentage of patients with TEAEs for injection site reactions is reported. For the period 1 'Baseline - Week 24', TEAEs were defined as AEs that started or worsened on or after first dose of trial medication and prior to date of the Week 24 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients who discontinued treatment before Week 24. For the period 2 'Week 24 - Week 46', TEAEs were defined as AEs that started or worsened on Week 24 visit and prior to or on Week 56 visit or within 10 weeks (70 days, inclusive) after last dose of trial medication for patients discontinuing treatment prior to Week 46. From first administration of trial medication until 10 weeks after last administration, up to a maximum of 56 weeks.
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