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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02100696
Other study ID # GA28950
Secondary ID 2013-004278-88
Status Completed
Phase Phase 3
First received
Last updated
Start date May 21, 2014
Est. completion date April 16, 2020

Study information

Verified date July 2021
Source Hoffmann-La Roche
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This Phase III, double-blind, placebo-controlled, multicenter study will investigate the efficacy and safety of etrolizumab during induction and maintenance of remission compared with placebo in the treatment of participants with moderately to severely active ulcerative colitis (UC) who have been previously exposed to TNF inhibitors.


Recruitment information / eligibility

Status Completed
Enrollment 609
Est. completion date April 16, 2020
Est. primary completion date April 16, 2020
Accepts healthy volunteers No
Gender All
Age group 18 Years to 80 Years
Eligibility Inclusion Criteria: - Diagnosis of UC established at least 3 months prior to Day 1 - Moderately to severely active UC as determined by the Mayo Clinic Score (MCS) assessment - Treatment within 5 years prior to screening with one or two induction regimens that contain TNF inhibitors (including TNF inhibitor biosimilars) - Washout of anti-TNF therapy for at least 8 weeks preceding Day 1 - Background regimen for UC may include oral 5-aminosalicylic acid (5-ASA), oral corticosteroids, budesonide, probiotics, azathioprine (AZA), 6-mercaptopurine (6-MP), or methotrexate (MTX) if doses have been stable during the screening period - Use of highly effective contraception as defined by the protocol - Must have received a colonoscopy within the past year or be willing to undergo a colonoscopy in lieu of a flexible sigmoidoscopy at screening Exclusion Criteria: - A history of or current conditions and diseases affecting the digestive tract, such as indeterminate colitis, suspicion of ischemic colitis, radiation colitis, or microscopic colitis, Crohn's disease, fistulas or abdominal abscesses, colonic mucosal dysplasia, intestinal obstruction, toxic megacolon, or unremoved adenomatous colonic polyps - Prior or planned surgery for UC - Past or present ileostomy or colostomy - Any prior treatment with etrolizumab or other anti-integrin agents (including natalizumab, vedolizumab, and efalizumab) - Any prior treatment with anti-adhesion molecules (e.g. anti-MAdCAM-1) - Any prior treatment with rituximab - Any treatment with tofacitinib during screening - Congenital or acquired immune deficiency, chronic hepatitis B or C infection, human immunodeficiency virus (HIV) positive, or history of tuberculosis (active or latent) - Evidence of or treatment for Clostridium difficile or clinically significant cytomegalovirus (CMV) colitis within 60 days prior to Day 1 - Evidence of or treatment for other intestinal pathogens within 30 days prior to Day 1 - History of recurrent opportunistic infections and/or severe disseminated viral infections - History of organ transplant - Any major episode of infection requiring treatment with intravenous (IV) antibiotics within 8 weeks prior to screening or oral antibiotics within 4 weeks prior to screening - Received a live attenuated vaccine within 4 weeks prior to Day 1

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Etrozulimab
Participants will receive 105 mg etrolizumab administered by SC injection Q4W.
Placebo
Participants will receive placebo (matched with etrolizumab) administered by SC injection Q4W.

Locations

Country Name City State
Argentina Hospital Provincial del Centenario Rosario
Australia St Vincent's Hospital Melbourne Fitzroy Victoria
Australia Footscray Hospital; Gastroenterology Footscray Victoria
Australia Royal Brisbane and Women's Hospital Herston Queensland
Australia Launceston General Hospital; Gastroenterology Research Launceston Tasmania
Australia St Frances Xavier Cabrini Hospital Malvern Victoria
Australia Fiona Stanley Hospital Murdoch Western Australia
Australia Mater Adult Hospital South Brisbane Queensland
Australia Princess Alexandra Hospital Woolloongabba Queensland
Austria Klinikum Klagenfurt am Wörtersee; Acute geriatric care Klagenfurt
Austria LKH - Universitätsklinikum der PMU Salzburg Salzburg
Austria Medizinische Universität Wien Wien
Belgium Imeldaziekenhuis Bonheiden
Belgium UZ Brussel Brussel
Belgium CHU St Pierre (St Pierre) Brussels
Belgium UZ Gent Gent
Belgium AZ Sint Elisabeth Herentals Herentals
Belgium UZ Leuven; Neurology Leuven
Belgium CHU de Liège; Tour de Pathologie Liège
Belgium AZ Delta (Stedelijk Ziekenhuis) Roeselare
Brazil Hospital Felicio Rocho Belo Horizonte MG
Brazil UNESP - Faculdade de Medicina da Universidade Estadual Paulista - Campus Botucatu Botucatu SP
Brazil CAEP - Centro Avancado de Estudos e Pesquisas Ltda. Campinas SP
Brazil Centro Digestivo de Curitiba Curitiba PR
Brazil Instituto Goiano de Gastroenterologia e Endoscopia Digestiva Ltda Goiânia GO
Brazil Hospital de Clínicas de Porto Alegre X Porto Alegre RS
Brazil Hospital Moinhos de Vento Porto Alegre RS
Brazil Hospital Universitario Clementino Fraga Filho - UFRJ Rio de Janeiro RJ
Brazil Hospital Estadual Mario Covas Santo Andre SP
Canada University of Calgary; Heritage Medical Research Clinic Calgary Alberta
Canada Zeidler Ledcor Centre - University of Alberta; Division of Gasroenterology Edmonton Alberta
Canada Queen Elizabeth II Health Sciences Centre; Gastroenterology Research Halifax Nova Scotia
Canada Hotel Dieu de Levis Levis Quebec
Canada Hôpital Maisonneuve - Rosemont Montreal Quebec
Canada Taunton Health Centre Oshawa Ontario
Canada Mount Sinai Hospital Toronto Ontario
Canada Toronto Liver Centre Toronto Ontario
Canada Pacific Gastroenterology Associates Vancouver British Columbia
Canada Toronto Digestive Disease Associates Vaughan Ontario
Czechia Fakultni nemocnice Brno; Interni kardiologicka klinika Brno
Czechia Hepato-Gastroenterologie HK, s.r.o. Hradec Kralove
Czechia Pardubicka krajska nemocnice, a.s. Pardubice
Czechia Nemocnice Na Bulovce Prague
Czechia ISCARE a.s. Praha 7
Czechia Krajska zdravotni, a.s. - Masarykova nemocnice v Usti nad Labem, o.z., Ocni oddeleni Usti Nad Labem
Denmark Ålborg Universitets Hospital; Gastromedicinsk Ålborg
Denmark Rigshospitalet; Medicinsk gastroenterologisk klinik København Ø
France CHU Amiens - Hopital Sud; Pharmacie - Secteur des Essais cliniques Amiens Cedex01
France Hôpital Beaujon Clichy cedex
France Hopital Claude Huriez - CHU Lille Lille
France Hôpital Nord - CHU Marseille; Gastroenterology and Hepatology Marseille cedex 20
France CHU Nice - Hopital de l'Archet 2 Nice
France Hôpital Saint-Louis Paris
France Groupe Hospitalier Sud - Hôpital Haut-Lévêque - USN Pessac
France CHU Saint Etienne - Hôpital Nord Saint Etienne
France Höpital Hautepierre; Pediatrie1 Strasbourg
France CHU de Toulouse - Hôpital Rangueil Toulouse Cedex 09
France Hôpital de Brabois Adultes Vandoeuvre-les-nancy
Germany Charite Universitaetsmedizin Berlin - Campus Charite Mitte Berlin
Germany DRK Kliniken Berlin Westend Berlin
Germany Universitaetsklinikum Erlangen Erlangen
Germany Klinikum der Johann Wolfgang Goethe-Universitaet Frankfurt
Germany Universitätsklinikum Freiburg; Innere Medizin I; Hämatologie, Onkologie und Stammzelltransplantation Freiburg
Germany Universitaetsklinikum Halle (Saale) Halle
Germany Gastroenterologie Eppendorfer Baum Hamburg
Germany Hamburgisches Forschungsinstitut fuer CED Hamburg
Germany Universitätsklinikum Hamburg-Eppendorf Hamburg
Germany Medizinische Hochschule Hannover; Klinik für Gastroenterologie, Hepatologie und Endokrinologie Hannover
Germany Universitaetsklinikum Schleswig-Holstein, Campus Kiel Kiel
Germany Klinikum Mannheim GmbH Universitätsklinikum Mannheim
Germany Universitaetsklinikum Muenster Muenster
Germany Universitaetsklinikum Ulm Ulm
Greece Anticancer Hospital of Thessaliniki " Theagenio" Thessaloniki
Hungary Bekes Megyei Kozponti Korhaz Dr. Rethy Pal Tagkorhaza Bekescsaba
Hungary Eszak-Kozep-budai Centrum, Uj Szent Janos Korhaz es Szakrendelo Budapest
Hungary Magyar Honvedseg Egeszsegugyi Kozpont; Fázis I-es Klinikai Farmakológiai Vizsgálóhely Budapest
Hungary Obudai Egeszsegugyi Centrum Kft. Budapest
Hungary Pannonia Maganorvosi Centrum Budapest
Hungary Semmelweis Egyetem Budapest
Hungary Debreceni Egyetem Debrecen
Hungary Markhot Ferenc Oktato Korhaz es Rendelointezet Eger
Hungary Petz Aladar Megyei Oktato Korhaz Gyor
Hungary Borsod-Abauj-Zemplen Megyei Korhaz es Egyetemi Oktato Korhaz; II. Belgyogyaszat Miskolc
Hungary Pecsi Tudomanyegyetem Pecs
Hungary Fejer Megyei Szent Gyorgy Egyetemi Oktato Korhaz Székesfehérvár
Israel Hadassah University Hospital - Ein Kerem; Neurosurgery Jerusalem
Israel Shaare Zedek Medical Center Jerusalem
Israel Rabin Medical Center-Beilinson Campus; Gaucher Clinic, Genetics Institute Petach Tiqwa
Israel Kaplan Medical Center Rehovot
Israel Assaf Harofeh Rishon Lezion
Italy Azienda Ospedaliera S. Orsola-Malpighi Bologna Emilia-Romagna
Italy Azienda Ospedaliera Universitaria Careggi Firenze Toscana
Italy Azienda Socio Sanitaria Territoriale Fatebenefratelli (Presidio Ospedale Sacco) Milano Lombardia
Italy A.O.U. Policlinico di Modena Modena Emilia-Romagna
Italy Azienda Ospedaliera Di Padova Padova Veneto
Italy Ospedale di Circolo; Neuropsichiatria Infantile Rho Lombardia
Italy Azienda Ospedaliera San Camillo Forlanini Roma Lazio
Italy Azienda Ospedaliera Universitaria Policlinico Tor Vergata Roma Lazio
Italy Fondazione Policlinico Universitario Agostino Gemelli IRCCS Roma Lazio
Italy Istituto Clinico Humanitas Rozzano (MI) Lombardia
Italy I.R.C.C.S Policlinico San Donato San Donato Milanese (MI) Lombardia
Korea, Republic of Kyungpook National University Hospital; Opthalmology Daegu
Korea, Republic of Korea University Ansan Hospital Gyeonggi-do
Korea, Republic of Seoul National University Bundang Hospital Seongnam-si
Korea, Republic of Asan Medical Center. Seoul
Korea, Republic of Samsung Medical Center Seoul
Korea, Republic of Seoul National University Hospital Seoul
Korea, Republic of Severance Hospital, Yonsei University Seoul
Korea, Republic of The Catholic University of Korea St. Vincent's Hospital Suwon-si,
Lithuania Hospital of Lithuanian University of Health. Sciences Kaunas Clinics Kaunas
Lithuania Vilnius University Hospital Santariskiu Clinic Public Insti Vilnius
Mexico Centro Regiomontano de Estudios Clínicos Roma S.C. Monterrey Nuevo LEON
Netherlands Amsterdam UMC Location AMC Amsterdam
Netherlands Amsterdam UMC, Locatie VUMC; Neurology Amsterdam
Netherlands Rijnstate; Internal Medicine Department Arnhem
Netherlands Radboudumc NL -nijmegen
Poland Nasz Lekarz Osrodek Badan Klinicznych Bydgoszcz
Poland Nzoz All-Medicus Katowice
Poland Gabinet Lekarski, Bartosz Korczowski Rzeszów
Poland Niepubliczny Zaklad Opieki Zdrowotnej SONOMED Szczecin
Poland Centrum Zdrowia MDM Warszawa
Poland Narodowy Instytut Onkologii im. Marii Sklodowskiej-Curie - Panstwowy Instytut Badawczy Warszawa
Poland Nzoz Vivamed Warszawa
Poland EuroMediCare Szpital Specjalistyczny z Przychodnia we Wroclawiu Wroclaw
Poland LexMedica Osrodek Badan Klinicznych Wroclaw
Poland PlanetMed Wroclaw
Romania SC Euroclinic Hospital SA Bucuresti
Spain Fundacion Hospital de Alcorcon; Servicio de Digestivo Alcorcon Madrid
Spain Hospital Universitari de Girona Dr Josep Trueta Girona
Spain Hospital Universitario de Fuenlabrada Madrid
Spain Hospital Universitario de la Princesa Madrid
Spain Hospital Universitari i Politecnic La Fe Valencia
Spain Hospital Universitario Miguel Servet Zaragoza
Switzerland Cliniques Universitaires Saint-Luc; Nephrology Bern
Switzerland Crohn-Colitis Zentrum Bern - Gemeinschaftspraxis Balsiger, Seibold und Partner Bern
Switzerland Inselspital-Universitaetsspital Bern; Institut fuer Spitalpharmazie Bern
United Kingdom Addenbrooke's Hospital Cambridge
United Kingdom Royal Devon and Exeter Hospital (Wonford) Exeter
United Kingdom King's College London London
United Kingdom St Thomas Hospital London
United Kingdom The Royal London Hospital London
United Kingdom University College London Hospital London
United Kingdom Fairfield General Hospital Manchester
United Kingdom Royal Victoria Infirmary Newcastle upon Tyne
United Kingdom Nottingham University Hospitals; QMC Campus Nottingham
United Kingdom Southampton General Hospital Southampton
United States University of Michigan; Michigan Institute for Clinical and Health Research (MICHR) Ann Arbor Michigan
United States Gastroenterology Associates, LLC Baton Rouge Louisiana
United States Washington Gastroenterology Bellevue Washington
United States University of Alabama at Birmingham Birmingham Alabama
United States Massachusetts General Hospital; Crohn's & Colitis Center Boston Massachusetts
United States University of North Carolina at Chapel Hill Chapel Hill North Carolina
United States Northwestern University Feinberg School Of Medicine Chicago Illinois
United States Consultants for Clinical Research Inc. Cincinnati Ohio
United States UC Health, LLC. Cincinnati Ohio
United States Ericksen Research and Development Clinton Utah
United States Rocky Mountain Gastroenterology Associates Denver Colorado
United States Henry Ford Health System Detroit Michigan
United States Clinica Peruano Americana S.A. Great Neck New York
United States Kansas City Research Institute, LLC Kansas City Missouri
United States University of California San Diego Medical Center La Jolla California
United States Rocky Mountain Gastroenterology Associates, P.L.L.C.; Gastroenterology Lakewood Colorado
United States Gastroenterology Associates of Central Georgia Macon Georgia
United States Gastrointestinal Specialists of Georgia, PC Marietta Georgia
United States Gastroenterology Center of the Midsouth, P.C. Memphis Tennessee
United States Great Lakes Gastroenterology Research, LLC Mentor Ohio
United States FQL Research, LLC Miramar Florida
United States Vanderbilt University Medical Center Nashville Tennessee
United States Weill Cornell Medical College-New York Presbyterian Hospital New York New York
United States Digestive and Liver Disease Specialists, Ltd. Norfolk Virginia
United States Southwest Gastroenterology Oak Lawn Illinois
United States Center For Digestive Health Orlando Florida
United States Internal Medicine Specialists Orlando Florida
United States McGuire Research Institute; Gastroenterology Richmond Virginia
United States University of Utah School of Medicine Salt Lake City Utah
United States Clinical Applications Laboratories, Inc. San Diego California
United States Precision Research Institute, LLC San Diego California
United States University of California at San Francisco San Francisco California
United States Louisiana Research Center, LLC Shreveport Louisiana
United States Atlanta Gastroenterology Specialists, PC Suwanee Georgia
United States Cotton-O'Neil Clinical Research Center, Digestive Health Topeka Kansas
United States Center for Digestive Health Troy Michigan
United States Tyler Research Institute, LLC Tyler Texas
United States Shafran Gastroenterology Center Winter Park Florida

Sponsors (1)

Lead Sponsor Collaborator
Hoffmann-La Roche

Countries where clinical trial is conducted

United States,  Argentina,  Australia,  Austria,  Belgium,  Brazil,  Canada,  Czechia,  Denmark,  France,  Germany,  Greece,  Hungary,  Israel,  Italy,  Korea, Republic of,  Lithuania,  Mexico,  Netherlands,  Poland,  Romania,  Spain,  Switzerland,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Induction Phase: Percentage of Participants With Remission at Week 14, as Determined by the Mayo Clinic Score (MCS) The Mayo Clinic Score (MCS) ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Remission was defined as MCS less than or equal to (=)2 with individual subscores =1 and a rectal bleeding subscore of 0. Week 14
Primary Maintenance Phase: Percentage of Participants With Remission at Week 66 Among Participants Who Had Achieved a Clinical Response at Week 14, as Determined by the MCS The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Remission was defined as MCS less than or equal to (=)2 with individual subscores =1 and a rectal bleeding subscore of 0. Clinical Response is MCS with =3-point decrease and 30% reduction from baseline as well as =1-point decrease in rectal bleeding subscore or an absolute rectal bleeding score of 0 or 1. Week 66
Secondary Induction Phase: Percentage of Participants With Clinical Remission at Week 14, as Determined by the MCS The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Clinical Remission is MCS =2 with individual subscores =1. Week 14
Secondary Induction Phase: Percentage of Participants With Clinical Response at Week 14, as Determined by the MCS The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Remission was defined as MCS less than or equal to (=)2 with individual subscores =1 and a rectal bleeding subscore of 0. Clinical Response is MCS with =3-point decrease and 30% reduction from baseline as well as =1-point decrease in rectal bleeding subscore or an absolute rectal bleeding score of 0 or 1. Week 14
Secondary Induction Phase: Percentage of Participants With Improvement From Baseline in Endoscopic Appearance of the Mucosa at Week 14, as Determined by the MCS Endoscopic Subscore The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Improvement in endoscopic appearance of the mucosa is Endoscopy subscore =1. Baseline and Week 14
Secondary Induction Phase: Percentage of Participants With Endoscopic Remission at Week 14, as Determined by the MCS Endoscopic Subscore The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Endoscopic Remission is Endoscopy subscore = 0. Week 14
Secondary Induction Phase: Percentage of Participants With Histologic Remission at Week 14, as Determined by the Nancy Histological Index Nancy Histological Index (NHI) is a 5-level classification ranging from grade 0 (No histologically significant disease) to grade 4 (severely active disease). Histologic remission is defined as a Nancy Histological Index of 0 or 1. Week 14
Secondary Induction Phase: Change From Baseline to Week 6 in MCS Rectal Bleed Subscore Rectal bleeding data were collected via the participant's diaries and each day a participant provided a score from 0 to 3 according to the following definitions: 0 = no blood in the stool; 1 = streaks of blood with stool less than half the time; 2 = obvious blood with stool most of the time; 3 = blood alone passed. The Mayo Clinic Score (MCS) rectal bleeding subscore was calculated as the worst value of three days of daily diary scores closest to anchor dates at baseline and post-baseline. The data was considered non-parametric and was reported using RANK analysis of covariance (ANCOVA). Participants were stratified by concomitant treatment with corticosteroids or immunosuppressants at randomization and disease activity measured during screening (MCS =9/MCS =10); the model adjusted for these stratification factors along with the baseline rectal bleeding (RB) subscore. Baseline and Week 6
Secondary Induction Phase: Change From Baseline to Week 6 in MCS Stool Frequency Subscore Stool frequency data were collected via the participant's diaries and each day a participant provided a score from 0 to 3 according to the following definitions: 0 = normal number of stools; 1 = 1 to 2 more stools than normal; 2 = 3 to 4 more stools than normal; 3 = 5 or more stools than normal. The Mayo Clinic Score (MCS) stool frequency subscore was calculated as the average of three days daily diary scores closest to anchor dates at baseline and post-baseline. The data was considered non-parametric and was reported using RANK analysis of covariance (ANCOVA). Participants were stratified by concomitant treatment with corticosteroids or immunosuppressants at randomization and disease activity measured during screening (MCS =9/MCS =10); the model adjusted for these stratification factors along with the baseline stool frequency (SF) subscore. Baseline and Week 6
Secondary Induction Phase: Change From Baseline to Week 14 in UC Bowel Movement Signs and Symptoms, as Assessed by the Ulcerative Colitis Patient-Reported Outcome Signs and Symptoms (UC-PRO/SS) Questionnaire The UC-PRO questionnaire is collected in the e-diary and completed by participants for at least 9-12 consecutive days prior to a study visit. The UC-PRO is being reported in three domains; two domains are key endpoints and reported as UC-PRO Signs and Symptoms (UC-PRO/SS). The bowel domain score ranges from 0-27, with a higher score indicating a worse disease state. Baseline and Week 14
Secondary Induction Phase: Change From Baseline to Week 14 in UC Functional Symptoms, as Assessed by the UC-PRO/SS Questionnaire The UC-PRO questionnaire is collected in the e-diary and completed by participants for at least 9-12 consecutive days prior to a study visit. The UC-PRO is being reported in three domains; two domains are key endpoints and reported as UC-PRO Signs and Symptoms (UC-PRO/SS). The functional (abdominal symptoms) domain score ranges from 0-12, with a higher score indicating a worse disease state. Baseline and Week 14
Secondary Induction Phase: Change From Baseline to Week 14 in Health-Related Quality of Life, as Assessed by the Overall Score of the Inflammatory Bowel Disease Questionnaire (IBDQ) The IBDQ score is a Total Score summed up from across all 32 questions on the questionnaire. The Total Score range is from 32 to 224 with higher scores representing a better quality of life. Baseline and Week 14
Secondary Maintenance Phase: Percentage of Participants With Clinical Remission at Week 66 Among Participants Who Had Achieved Clinical Remission at Week 14, as Determined by the MCS The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Remission was defined as MCS less than or equal to (=)2 with individual subscores =1 and a rectal bleeding subscore of 0. Clinical Remission is MCS =2 with individual subscores =1. Week 66
Secondary Maintenance Phase: Percentage of Participants With Clinical Remission at Week 66, as Determined by the MCS The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Remission was defined as MCS less than or equal to (=)2 with individual subscores =1 and a rectal bleeding subscore of 0. Clinical Remission is MCS =2 with individual subscores =1. Week 66
Secondary Maintenance Phase: Percentage of Participants With Remission at Week 66 Among Participants Who Had Achieved Remission at Week 14, as Determined by the MCS The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Remission was defined as MCS less than or equal to (=)2 with individual subscores =1 and a rectal bleeding subscore of 0. Week 66
Secondary Maintenance Phase: Percentage of Participants With Improvement From Baseline in Endoscopic Appearance of the Mucosa at Week 66, as Determined by the MCS Endoscopic Subscore The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Improvement in endoscopic appearance of the mucosa is Endoscopy subscore =1. Baseline and Week 66
Secondary Maintenance Phase: Percentage of Participants With Histologic Remission at Week 66, as Determined by the Nancy Histological Index Nancy Histological Index (NHI) is a 5-level classification ranging from grade 0 (No histologically significant disease) to grade 4 (severely active disease). Histologic remission is defined as a Nancy Histological Index of 0 or 1. Week 66
Secondary Maintenance Phase: Percentage of Participants With Endoscopic Remission at Week 66, as Determined by the MCS Endoscopic Subscore The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Endoscopic Remission is Endoscopy subscore = 0. Week 66
Secondary Maintenance Phase: Percentage of Participants With Corticosteroid-Free Clinical Remission at Week 66 Among Participants Who Were Receiving Corticosteroids at Baseline, as Determined by the MCS The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Corticosteroid-Free analysis was conducted only on a subgroup of participants who were randomized into the maintenance phase and receiving Corticosteroids (CS) at baseline. Participants were defined as being off CS if they had no record of taking CS on the date that was 24 weeks prior to Week 66. Week 66
Secondary Maintenance Phase: Percentage of Participants With Corticosteroid-Free Remission at Week 66 Among Participants Who Were Receiving Corticosteroids at Baseline, as Determined by the MCS The MCS ranges from 0 to 12 and is a composite of 4 assessments (each rated from 0-3): stool frequency, rectal bleeding, endoscopy, and physician's global assessment. Higher scores represent greater disease severity. Corticosteroid-Free analysis was conducted only on a subgroup of participants who were randomized into the maintenance phase and receiving Corticosteroids (CS) at baseline. Participants were defined as being off CS if they had no record of taking CS on the date that was 24 weeks prior to Week 66. Week 66
Secondary Maintenance Phase: Change From Baseline to Week 66 in UC Bowel Movement Signs and Symptoms, as Assessed by the UC-PRO/SS Questionnaire The UC-PRO questionnaire is collected in the e-diary and completed by participants for at least 9-12 consecutive days prior to a study visit. The UC-PRO is being reported in three domains; two domains are key endpoints and reported as UC-PRO Signs and Symptoms (UC-PRO/SS). The bowel domain score ranges from 0-27, with a higher score indicating a worse disease state. Baseline and Week 66
Secondary Maintenance Phase: Change From Baseline to Week 66 in UC Functional Symptoms, as Assessed by the UC-PRO/SS Questionnaire The UC-PRO questionnaire is collected in the e-diary and completed by participants for at least 9-12 consecutive days prior to a study visit. The UC-PRO is being reported in three domains; two domains are key endpoints and reported as UC-PRO Signs and Symptoms (UC-PRO/SS). The functional (abdominal symptoms) domain score ranges from 0-12, with a higher score indicating a worse disease state. Baseline and Week 66
Secondary Maintenance Phase: Change From Baseline to Week 66 in Health-Related Quality of Life, as Assessed by the Overall Score of the IBDQ The IBDQ is used to assess participant's health-related quality of life (QOL). The IBDQ score is a Total Score summed up from across all 32 questions on the questionnaire. The Total Score range is from 32 to 224 with higher scores representing a better quality of life. Baseline and Week 66
Secondary Number of Participants With at Least One Adverse Event by Severity, According to National Cancer Institute Common Terminology Criteria for Adverse Events, Version 4.0 (NCI-CTCAE v4.0) All Adverse Events (AEs) were graded for severity using the NCI-CTCAE v4.0. Any AE not specifically listed was assessed per the following 5 grades: Grade 1 = mild; asymptomatic or mild symptoms; clinical or diagnostic observations only; or intervention not indicated. Grade 2 = moderate; minimal, local, or non-invasive intervention indicated; or limiting age-appropriate instrumental activities of daily living. Grade 3 = severe or medically significant, but not immediately life-threatening; hospitalization or prolongation of hospitalization indicated; disabling; or limiting self-care activities of daily living. Grade 4 = life-threatening consequences or urgent intervention indicated. Grade 5 = death related to AE. Not all grades are appropriate for all AEs; some AEs have fewer than 5 options. The terms "severe" and "serious" are not synonymous and are independently assessed for each AE. Multiple occurrences of AEs were counted only once per participant at the highest (worst) grade. From Baseline up to Week 78
Secondary Number of Participants With Adverse Events Leading to Study Drug Discontinuation From Baseline up to Week 78
Secondary Number of Participants With Serious Infection-Related Adverse Events From Baseline up to Week 78
Secondary Number of Participants With Infection-Related Adverse Events All Adverse Events (AEs) were graded for severity using the NCI-CTCAE v4.0. Any AE not specifically listed was assessed per the following 5 grades: Grade 1 = mild; asymptomatic or mild symptoms; clinical or diagnostic observations only; or intervention not indicated. Grade 2 = moderate; minimal, local, or non-invasive intervention indicated; or limiting age-appropriate instrumental activities of daily living. Grade 3 = severe or medically significant, but not immediately life-threatening; hospitalization or prolongation of hospitalization indicated; disabling; or limiting self-care activities of daily living. Grade 4 = life-threatening consequences or urgent intervention indicated. Not all grades are appropriate for all AEs; some AEs have fewer than 5 options. The terms "severe" and "serious" are not synonymous and are independently assessed for each AE. Multiple occurrences of AEs were counted only once per participant at the highest (worst) grade. From Baseline up to Week 78
Secondary Number of Participants With Injection-Site Reaction-Related Adverse Events From Baseline up to Week 78
Secondary Number of Participants With Hypersensitivity Reaction-Related Adverse Events From Baseline up to Week 78
Secondary Number of Participants With Malignancies From Baseline up to Week 78
Secondary Number of Participants With Anti-Therapeutic Antibodies to Etrolizumab at Baseline and During the Study A tiered strategy was used to detect and characterize etrolizumab antibodies within this clinical study. When determining post baseline incidence, participants were considered to be ADA positive if they were ADA negative or had missing data at baseline but developed an ADA response following etrolizumab drug exposure (treatment-induced ADA response), or if they were ADA positive at baseline and the titer of one or more post baseline samples was at least 0.60 titer unit greater than the titer of the baseline sample (treatment-enhanced ADA response). Participants were considered to be ADA negative if they were ADA negative or had missing data at baseline and all post baseline samples were negative, or if they were ADA positive at baseline but did not have any post baseline samples with a titer that was at least 0.60 titer unit greater than the titer of the baseline sample (treatment unaffected). Pre-dose at Baseline, Weeks 4, 14, 24, 44, and 66, and Early Termination/End of Safety Follow-Up (up to Week 78)
Secondary Etrolizumab Serum Trough Concentration (for Arms/Timepoints Above LLOQ) As per Protocol, the timepoints for each arm where more than a third of the samples were above the lower limit of quantification (LLOQ), full summary statistics (Mean and Standard Deviation) were reported. For timepoints below the LLOQ, only the Median and Max were reported as a separate outcome measure below. Pre-dose (0 hour) at Baseline and Weeks 14, 24, 44 and 66
Secondary Etrolizumab Serum Trough Concentration (for Arms/Timepoints Below LLOQ) As per Protocol, the timepoints for each arm where more than a third of the samples were below the LLOQ only the Median and Max were reported. Weeks 44 and 66
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