A Study of Ocrelizumab in Comparison With Interferon Beta-1a (Rebif) in Participants With Relapsing Multiple Sclerosis

• ClinicalTrials.gov Identifier: NCT01412333
• Recruitment Status: Completed
• First Posted: August 9, 2011
• Results First Posted: July 18, 2017
• Last Update Posted: March 3, 2023
• Sponsor: Hoffmann-La Roche
• Information provided by (Responsible Party): Hoffmann-La Roche

Study Description

Brief Summary:

This randomized, double-blind, double-dummy, parallel-group study will evaluate the efficacy and safety of ocrelizumab in comparison with interferon beta-1a (Rebif) in participants with relapsing multiple sclerosis. Participants will be randomized to receive either ocrelizumab 600 mg or matching placebo intravenous (IV) as 300 mg infusions on Days 1 and 15 for the first dose and as a single infusion of 600 mg for all subsequent infusions every 24 weeks, with placebo injections matching interferon beta-1a SC three times per week; or interferon beta-1a 44 mcg SC injections three times per week (with placebo infusions matching ocrelizumab infusions every 24 weeks).

Condition or disease	Intervention/treatment	Phase
Relapsing Multiple Sclerosis	Drug: Interferon beta-1a; Drug: Ocrelizumab-matching placebo; Drug: Ocrelizumab; Drug: Interferon beta-1a-matching placebo	Phase 3

Study Design

• Study Type: Interventional (Clinical Trial)
• Actual Enrollment: 835 participants
• Allocation: Randomized
• Intervention Model: Parallel Assignment
• Masking: Triple (Participant, Investigator, Outcomes Assessor)
• Primary Purpose: Treatment
• Official Title: A Randomized, Double-Blind, Double-Dummy, Parallel-Group Study To Evaluate the Efficacy and Safety of Ocrelizumab in Comparison to Interferon Beta-1a (Rebif) in Patients With Relapsing Multiple Sclerosis
• Actual Study Start Date: September 20, 2011
• Actual Primary Completion Date: May 12, 2015
• Actual Study Completion Date: December 30, 2022

Arms and Interventions

Arm	Intervention/treatment
Active Comparator: Interferon beta-1a 44 mcg SC; Interferon beta-1a 44 mcg SC injections three times per week (with placebo infusions matching ocrelizumab infusions every 24 weeks).	Drug: Interferon beta-1a; Other Name: Rebif; Drug: Ocrelizumab-matching placebo
Experimental: Ocrelizumab; Ocrelizumab 600 mg or matching placebo intravenous (IV) as 300 mg infusions on Days 1 and 15 for the first dose and as a single infusion of 600 mg for all subsequent infusions every 24 weeks, with placebo injections matching interferon beta-1a SC three times per week.	Drug: Ocrelizumab; Other Name: RO4964913; Drug: Interferon beta-1a-matching placebo

Outcome Measures

Primary Outcome Measures :

1. Annualized Relapse Rate (ARR) in Participants With Relapsing Multiple Sclerosis (MS) at 96 Weeks [ Time Frame: Week 96 ]
   ARR was protocol-defined and calculated as the total number of relapses for all participants in the treatment group divided by the total participant-years of exposure to that treatment.

Secondary Outcome Measures :

1. Time to Onset of Confirmed Disability Progression (CDP) for at Least 12 Weeks During the Double-Blind Treatment Period [ Time Frame: Week 104 ]
   Disability progression was defined as an increase in the Expanded Disability Status Scale (EDSS) score of: A) >=1.0 point from the baseline EDSS score when the baseline score was less than or equal to (<=) 5.5 B) >=0.5 point from the baseline EDSS score when the baseline score was >5.5 The EDSS scale ranges from 0 (normal neurological exam) to 10 (death due to multiple sclerosis). This outcome measure was considered confirmatory only when results of both studies WA21092 and WA21093 were combined. Disability progression was considered confirmed when the increase in the EDSS was confirmed at a regularly scheduled visit at least 12 weeks after the initial documentation of neurological worsening. Participants who had initial disability progression with no confirmatory EDSS assessment and who were on treatment at time of clinical cut-off date were censored at the date of their last EDSS assessment.
2. Number of T1 Gadolinium (Gd)-Enhancing Lesions as Detected by Brain Magnetic Resonance Imaging (MRI) During the Double-Blind Treatment [ Time Frame: Baseline up to week 96 ]
   The total number of T1 gadolinium-enhancing lesions for all participants in the treatment group was calculated as the sum of the individual number of lesions at Weeks 24, 48, and 96.
3. Number of New, and/or Enlarging T2 Hyperintense Lesions as Detected by Brain Magnetic Resonance Imaging (MRI) During the Double Blind Treatment [ Time Frame: Baseline up to week 96 ]
   The total number of new and/or enlarging T2 lesions for all participants in the treatment group was calculated as the sum of the individual number of lesions at Weeks 24, 48, and 96.
4. Percentage of Participants With Confirmed Disability Improvement (CDI) for at Least 12 Weeks [ Time Frame: Week 96 ]
   Disability improvement was assessed only for the subgroup of participants with a baseline EDSS score of >= 2.0. It was defined as a reduction in EDSS score of: A) >=1.0 from the baseline EDSS score when the baseline score was >=2 and <=5.5 B) >= 0.5 when the baseline EDSS score > 5.5. The EDSS scale ranges from 0 (normal neurological exam) to 10 (death due to multiple sclerosis). This outcome measure was considered confirmatory only when results of both studies WA21092 and WA21093 were combined.
5. Time to Onset of Confirmed Disability Progression (CDP) for at Least 24 Weeks During the Double-Blind Treatment Period [ Time Frame: Week 104 ]
   Disability progression was defined as an increase in the Expanded Disability Status Scale (EDSS) score of: A) >=1.0 point from the baseline EDSS score when the baseline score was less than or equal to (<=) 5.5 B) >=0.5 point from the baseline EDSS score when the baseline score was >5.5 The EDSS scale ranges from 0 (normal neurological exam) to 10 (death due to multiple sclerosis). This outcome measure was considered confirmatory only when results of both studies WA21092 and WA21093 were combined. Disability progression was considered confirmed when the increase in the EDSS was confirmed at a regularly scheduled visit at least 24 weeks after the initial documentation of neurological worsening. Participants who had initial disability progression with no confirmatory EDSS assessment and who were on treatment at time of clinical cut-off date were censored at the date of their last EDSS assessment.
6. Number of T1 Hypointense Lesions During the Double-Blind Treatment [ Time Frame: Baseline up to week 96 ]
   The total number of new T1-Hypo-Intense Lesions (Chronic Black Holes) for all participants in the treatment group was calculated as the sum of the individual number of new lesions at Weeks 24, 48, and 96.
7. Change From Baseline in Multiple Sclerosis Functional Composite (MSFC) Score to Week 96 [ Time Frame: Baseline, Week 96 ]
   MSFC score consists of: A) Timed 25-Foot walk; B) 9-Hole Peg Test (9-HPT); and C) Paced Auditory Serial Addition Test (PASAT-3 version). The MSFCS is based on the concept that scores for these three dimensions (arm, leg, and cognitive function) are combined to create a single score (the MSFC) that can be used to detect change over time in a group of participants with MS. Since the three primary measures differ in what they actually measure, a common composite score for the three different measures i.e., Z- score was selected for the purpose. MSFC Score = {Z arm, average + Z leg, average + Z cognitive} / 3.0. The results from each of these three tests are transformed into Z-scores and averaged to yield a composite score for each participant at each time point. A score of +1 indicates that, on average, an individual scored 1 standard deviation (SD) better than the reference population and a score of -1 indicates that an individual scored 1 SD worse than the reference population.
8. Percent Change in Brain Volume as Detected by Brain Magnetic Resonance Imaging (MRI) From Week 24 to Week 96 [ Time Frame: From week 24 up to week 96 ]
   Brain volume was recorded as an absolute "normalized" value at the baseline visit then recorded at subsequent visits as a percentage change relative to the absolute value at the baseline visit. Therefore, brain volume at Week 24 was calculated as the brain volume at the baseline visit multiplied by 1 + ([percentage change in brain volume from baseline visit to Week 24]/100). Estimates are from analysis based on mixed-effect model of repeated measures (MMRM) using unstructured covariance matrix: Percentage Change = Brain Volume at Week 24 + Geographical Region (US vs. ROW) + Baseline EDSS (< 4.0 vs. >= 4.0) + Week + Treatment + Treatment*Week (repeated values over Week) + Brain Volume at Week 24*Week. The EDSS scale ranges from 0 (normal neurological exam) to 10 (death due to multiple sclerosis).
9. Change From Baseline in Short Form Health Survey-36 (SF-36) Physical Component Summary (PCS) Score at Week 96 [ Time Frame: Baseline, Week 96 ]
   The SF-36 is a multi-purpose, short-form health survey with 36 questions. It yields an 8-scale profile of functional health and well-being scores (domains) as well as psychometrically based physical and mental health summary measures. The SF-36 taps 8 health concepts: physical functioning, bodily pain, physical role functioning, emotional role functioning, emotional well-being, social functioning, vitality, and general health perceptions. The 8 scales are further summarized to 2 distinct higher-ordered clusters: the PCS and mental composite t-score (MCS). The range for all 8 domains as well as for the composite t- scores is from 0 to 100 with 100 as best possible health status and 0 as worst health status.
10. Percentage of Participants Who Have No Evidence of Disease Activity (NEDA) up to Week 96 [ Time Frame: Week 96 ]
    NEDA was defined only for participants with a baseline EDSS score >=2.0. The EDSS scale ranges from 0 (normal neurological exam) to 10 (death due to multiple sclerosis). Participants who completed the 96- week treatment period were considered as having evidence of disease activity if at least one protocol- defined relapse (PDR), a confirmed disability progression (CDP) event or at least one MRI scan showing MRI activity (defined as Gd-enhancing T1 lesions, or new or enlarging T2 lesions) was reported during the 96-week treatment period, otherwise the participant was considered as having NEDA.
11. Number of Participants With Adverse Events (AEs) [ Time Frame: Baseline up to Week 96 ]
    AEs included infusion related reactions (IRRs) and serious MS relapses, but excluded non-serious MS relapses. Serious Adverse Events (SAEs) included serious MS relapses and serious IRRs.
12. Exposure to Ocrelizumab (Area Under the Concentration - Time Curve, AUC) [ Time Frame: Pre-infusion at Weeks 1, 24, 48, 72; and 30 minutes post-infusion at Week 72; at any time during Weeks 84 and 96 ]
    AUC represents total drug exposure for one dosing interval after the 4th dose.
13. Number of Participants With Anti-Drug Antibodies (ADAs) to Ocrelizumab [ Time Frame: Baseline up to Week 96 ]
    Number of participants positive for anti-drug antibodies (ADAs) to ocrelizumab is the number of post- baseline evaluable participants determined to have treatment-induced ADA or treatment-enhanced ADA during the study period.

Eligibility Criteria

• Ages Eligible for Study: 18 Years to 55 Years (Adult)
• Sexes Eligible for Study: All
• Accepts Healthy Volunteers: No

Criteria

Inclusion Criteria:

• Diagnosis of multiple sclerosis, in accordance with the revised McDonald criteria (2010)
• At least 2 documented clinical attacks within the last 2 years prior to screening or one clinical attack in the years prior to screening (but not within 30 days prior to screening)
• Neurologic stability for greater than or equal to (>/=) 30 days prior to both screening and baseline
• Expanded Disability Status Scale (EDSS) score 0 to 5.5 inclusive

Exclusion Criteria:

• Primary progressive multiple sclerosis
• Disease duration of more than 10 years in patients with EDSS score less than or equal to (</=) 2.0 at screening
• Contraindications for MRI
• Known presence of other neurological disorders which may mimic multiple sclerosis
• Pregnancy or lactation
• Requirement for chronic treatment with systemic corticosteroids or immunosuppressants during the course of the study
• History of or currently active primary or secondary immunodeficiency
• History of severe allergic or anaphylactic reactions to humanized or murine monoclonal antibodies
• Active infection, or history of or known presence of recurrent or chronic infection (for example, hepatitis B or C, Human Immunodeficiency Virus [HIV], syphilis, tuberculosis)
• History of progressive multifocal leukoencephalopathy
• Contraindications to or intolerance of oral or IV corticosteroids
• Contraindications to Rebif or incompatibility with Rebif use

Contacts and Locations

Locations

United States, Arizona

Hope Research Institute

Phoenix, Arizona, United States, 85050

HonorHealth Neurology

Scottsdale, Arizona, United States, 85251

Territory Neurology and Research Institute

Tucson, Arizona, United States, 85704

United States, California

Collaborative Neuroscience Research, LLC

Long Beach, California, United States, 90806

Stanford University Medical Center

Palo Alto, California, United States, 94304

United States, Colorado

University of Colorado

Denver, Colorado, United States, 80262

Advanced Neurosciences Research LLC

Fort Collins, Colorado, United States, 80528

United States, Connecticut

Associated Neurologists of Southern CT PC

Fairfield, Connecticut, United States, 06824

United States, Florida

Infinity Clinical Research

Hollywood, Florida, United States, 33024

University of Miami; Dept. of Neurology MS Center

Miami, Florida, United States, 33136

Neurological Services of Orlando

Orlando, Florida, United States, 32806

Lovelace Scientific Resources

Sarasota, Florida, United States, 34292

University of South Florida

Tampa, Florida, United States, 33612

United States, Georgia

Atlanta Neuroscience Institute

Atlanta, Georgia, United States, 30327

United States, Indiana

Josephson Wallack Munshower Neurology PC

Indianapolis, Indiana, United States, 46256

United States, Kansas

University of Kansas Medical Center

Kansas City, Kansas, United States, 66160

MidAmerica Neuroscience Institute

Prairie Village, Kansas, United States, 66206

United States, Kentucky

Associates in Neurology PSC

Lexington, Kentucky, United States, 40513

United States, Massachusetts

Dragonfly Research, LLC

Wellesley, Massachusetts, United States, 02481

University of Massachusetts Memorial Medical Center

Worcester, Massachusetts, United States, 01655

United States, Michigan

University of Michigan Health System

Ann Arbor, Michigan, United States, 48109-0666

Wayne State University; Department of Neurology

Detroit, Michigan, United States, 48201

United States, Minnesota

The Minneapolis Clinic of Neurology

Golden Valley, Minnesota, United States, 55422

United States, New Jersey

Rutgers New Jersey Medical School

Newark, New Jersey, United States, 07103

Holy Name Hospital

Teaneck, New Jersey, United States, 07666

MS Comprehensive Care Center

Teaneck, New Jersey, United States, 07666

Shore Neurology

Toms River, New Jersey, United States, 08755

United States, New York

Empire Neurology, PC

Latham, New York, United States, 12210

Weill Cornell MC-NY Presbyter; Dept. of Neurology/Neuroscience, Judith Jaffe Multiple Sclerosis Ctr

New York, New York, United States, 63110

South Shore Neurologic Associates P.C.

Patchogue, New York, United States, 11772

University of Rochester Medical Center

Rochester, New York, United States, 14642

SUNY at Stony Brook

Stony Brook, New York, United States, 11790

United States, North Carolina

The Neurological Institute PA

Charlotte, North Carolina, United States, 28204

Neurology Associates PA

Hickory, North Carolina, United States, 28602

Raleigh Neurology Associates

Raleigh, North Carolina, United States, 27607-6520

United States, Ohio

Columbus Neuroscience

Columbus, Ohio, United States, 43801

United States, Pennsylvania

Abington Neurological Associates

Abington, Pennsylvania, United States, 19001

United States, South Carolina

Absher Neurology PA

Greenville, South Carolina, United States, 29607

United States, Tennessee

Neurology Clinic PC

Cordova, Tennessee, United States, 38018

Sibyl Wray MD Neurology PC

Knoxville, Tennessee, United States, 37934

Advanced Neurosciences Institute

Nashville, Tennessee, United States, 37205

United States, Texas

University of Texas Southwestern Medical Center

Dallas, Texas, United States, 75390

Baylor College of Medicine

Houston, Texas, United States, 77030

Bhupesh Dihenia M.D. P.A.

Lubbock, Texas, United States, 79410

Central Texas Neurology Consultants

Round Rock, Texas, United States, 78681

Integra Clinical Research, Llc

San Antonio, Texas, United States, 78229

Neurology Center of San Antonio

San Antonio, Texas, United States, 78258

United States, Washington

Swedish Neuroscience Institute

Seattle, Washington, United States, 98122

Argentina

ALPI-Inst. de Rehabilitacion Marcelo Fitte

Buenos Aires, Argentina, C1425BWO

STAT Research S.A.

Ciudad de Buenos Airesa, Argentina, C1013AAB

Belarus

Grodno State Medical University

Grodno, Belarus, 230017

City Clinical Hospital #9

Minsk, Belarus, 220116

Vitebsk; Regional Diagnostic Center

Vitebsk, Belarus, 210023

Vitebsk Regional Clinical Hospital

Vitebsk, Belarus, 210032

Belgium

UZ Antwerpen

Edegem, Belgium, 2650

Bosnia and Herzegovina

University Clinic Ctr Sarajevo

Sarajevo, Bosnia and Herzegovina, 71 000

Uni Hospital Center Tuzla

Tuzla, Bosnia and Herzegovina, 75000

Brazil

Santa Casa de Misericordia; de Belo Horizonte

Belo Horizonte, MG, Brazil, 30150-221

Hospital Universitario Gaffree e Guinle

Rio de Janeiro, RJ, Brazil, 20270-004

Hospital das Clinicas - UNICAMP

Campinas, SP, Brazil, 13083-887

Bulgaria

MHATNP Sv.Naum EAD; Clinic for intensive treatment of neurology diseases

Sofia, Bulgaria, 1113

Fifth MHAT-Sofia AD; Neuro Dept with Vascular Unit

Sofia, Bulgaria, 1233

MHAT National Cardiology Hospital, EAD; Neurology

Sofia, Bulgaria, 1309

UMHAT Alexandrovska, EAD; Neurology

Sofia, Bulgaria, 1431

Canada, Alberta

Multiple Sclerosis Clinic

Calgary, Alberta, Canada, T2N 2T9

University of Alberta; Northern Alberta Trials & Research Centre

Edmonton, Alberta, Canada, T6G 2C8

Canada, British Columbia

Vancouver Hospital - UBC Hospital Site

Vancouver, British Columbia, Canada, V6Z 1Y6

Canada, Ontario

The Ottawa Hospital - General Campus

Ottawa, Ontario, Canada, K1H 8L6

Canada, Quebec

Clinique NeuroOutaouais

Gatineau, Quebec, Canada, J8Y 1W2

Recherche Sepmus Inc.

Greenfield Park, Quebec, Canada, J4V 2J2

Montreal Neurological Institute and Hospital

Montreal, Quebec, Canada, H3A 2B4

Hôpital Maisonneuve - Rosemont; Recherche Clinique de Neurologie

Montréal, Quebec, Canada, H1T 2M4

Croatia

General Hospital Pula

Pula, Croatia, 52100

General Hospital Varazdin

Varazdin, Croatia, 42000

Clinical Hospital Centre Zagreb;Clinic for Neurology

Zagreb, Croatia, 10000

Uni Hospital Centre Dubrava

Zagreb, Croatia, 10000

Czechia

Fakultni nemocnice Brno

Brno, Czechia, 613 00

Neurospol s.r.o.

Havirov, Czechia, 736 00

Pardubicka Krajska Nemocnice; Department of Neurology

Pardubice, Czechia, 532 03

Krajska zdravotni, a. s. ? Nemocnice Teplice, o. z.; Neurologicke oddeleni

Teplice, Czechia, 415 29

France

Hopital Neurologique Pierre Wertheimer

Bron, France, 69500

Hôpital General - Service de neurologie; Service de neurologie

Dijon Cedex, France, 21079

Hôpital Saint Philibert

Lommé, France, 59462

Groupe Hospitalier Pitie-Salpetriere

Paris, France, 75651

Hôpital Maison Blanche; Service de Neurologie

Reims, France, 51092

CHU toulouse - Hôpital Purpan; Departement de Neurologie

Toulouse, France, 31059

Germany

Sankt Gertrauden Krankenhaus; Neurologisches Facharztzentrum

Berlin, Germany, 10713

Neurologische Praxis Bonn

Bonn, Germany, 53117

Universitätsklinikum Düsseldorf; Klinik für Neurologie

Düsseldorf, Germany, 40225

Zentrum fuer ambulante Neurologie

Essen, Germany, 45138

Universitaetsklinikum Frankfurt; Klinik für Neurologie

Frankfurt, Germany, 60528

Universitaetsklinikum Heidelberg

Heidelberg, Germany, 69120

Ratsapotheke Mittweida

Mittweida, Germany, 09648

Klinikum Grosshadern der LMU

Muenchen, Germany, 81377

Klinikum rechts der Isar der TU Muenchen; Neurologische Klinik und Poliklinik im Neuro-Kopf-Zentrum

München, Germany, 81675

Neurologische Gemeinschaftspraxis Dr. Lang, Prof. Schreiber, Dr. Krauß, Dr. Kornhuber

Ulm, Germany, 89073

Ireland

St Vincents University Hospital

Dublin 4, Ireland

Italy

Azienda Ospedaliera Universitaria Policlinico Tor Vergata

Roma, Lazio, Italy, 00133

Policlinico Universitario Agostino Gemelli

Roma, Lazio, Italy, 00168

A.O. Universitaria S. Martino Di Genova

Genova, Liguria, Italy, 16132

Fondazione IRCCS Istituto Neurologico Carlo Besta; Farmacia Interna

Milano, Lombardia, Italy, 20133

Ospedale Civile di Montichiari; Centro Sclerosi Multipla

Montichiari, Lombardia, Italy, 25018

Azienda Ospedaliero Universitaria Ospedali Riuniti Umberto I-G.M. Lancisi-G. Salesi Di Ancona

Torrette - Ancona, Marche, Italy, 60100

Ospedale degli Infermi

Ponderano, Piemonte, Italy, 13875

Ospedale Generale Regionale F. Miulli

Acquaviva delle Fonti, Puglia, Italy, 70021

Ospedale Casa Sollievo Della Sofferenza IRCCS

San Giovanni Rotondo, Puglia, Italy, 71013

Fond. Ist. S. Raffaele - giglio

Cefalu, Sicilia, Italy, 90015

Mexico

Mexico Centre for Clinical Research

Ciudad de México, Mexico CITY (federal District), Mexico, 03100

Clinical Research Institute

Tlalnepantla de Baz, Mexico CITY (federal District), Mexico, 54055

Instituto Biomedico De Investigacion A.C.

Aguascalientes, Mexico, 20127

Hospital CIMA Chihuahua; Centro de Investigación Clínicatorre de Consultoriospiso 4

Chihuahua, Mexico, 31238

Hospital Angeles Culiacan; Neurociencias

Culiacan, Mexico, 80020

Hospital Mexico Americano SC; Departamento de Electroencefalografía

Guadalajara, Mexico, 44620

Norway

Haukeland Universitetssykehus

Bergen, Norway, 5053

Poland

Vitamed

Bydgoszcz, Poland, 85-021

MA-LEK Clinical Sp. Z o.o.

Katowice, Poland, 40-595

Krakowska Akademia Neurologii Sp z o.o. Centrum Neurologii K

Krakow, Poland, 31-505

SPZOZ Uniwersytecki Szp. Klin. nr1 im.N.Barlickiego UM;Oddzial Kliniczny Neurologii

Lodz, Poland, 90-153

Centrum Neurologii Krzysztof Selmaj

Lodz, Poland, 90-324

Samodz.Publi.Szpital Kliniczny; nr 4 w Lublinie

Lublin, Poland, 20-954

Wojewodzki Specjalistyczny Szpital w Olsztynie; Oddzial Neurologiczny z Pododdzialem Udarowym

Olsztyn, Poland, 10-561

Neuro-Care Gabriela Klodowska

Siemianowice ?l?skie, Poland, 41-100

mMED Maciej Czarnecki

Warszawa, Poland, 01-684

Russian Federation

State institution of health care - Territorial Clinical Hospital

Barnaul, Russian Federation, 656024

State autonomous institution of healthcare Inter-regional clinical and diagnostic center

Kazan, Russian Federation, 420101

Kirov City Clinical Hospital #1; Neurology Department

Kirov, Russian Federation, 610014

SBHI of Nizhny Novgorod region City Clinical Hospital #3; neurology department

Nizniy Novgorod, Russian Federation, 603155

Perm SMA n.a. academ. E.A. Vagner

Perm, Russian Federation, 614990

City Clinical Hospital#2

Pyatigorsk, Russian Federation, 357538

St. Petersburg State Medical University n.a. I.P. Pavlov; Hematology, transfusiology and transplanta

Saint-Petersburg, Russian Federation, 197022

Saratov State Medical University of RosZdrav; Neurology

Saratov, Russian Federation, 410012

Slovakia

MUDr. Beata Dupejova Neurologicka ambulancia s.r.o

Banska Bystrica, Slovakia, 974 04

Fakultna Nemocnica Roosevelta

Banska Bystrica, Slovakia, 975 17

Vseobecna nemocnica s poliklinikou Levoca a.s.

Levoca, Slovakia, 054 01

Spain

Institut Catala d?Oncologia Hospital Germans Trias i Pujol

Badalona, Barcelona, Spain, 08916

Hospital Universitari de Bellvitge; Servicio de Neurologia

L'Hospitalet de Llobregat, Barcelona, Spain, 08907

Hospital General Univ. de Alicante

Alicante, Spain, 03010

Hospital del Mar

Barcelona, Spain, 08003

Hospital Universitari Vall d'Hebron

Barcelona, Spain, 08035

Hospital Universitari de Girona Dr Josep Trueta

Girona, Spain, 17007

Hospital General Universitario Gregorio Marañon; Servicio de Neurologia

Madrid, Spain, 28007

Hospital Universitario Clinico San Carlos

Madrid, Spain, 28040

Hospital Regional Universitario de Malaga

Malaga, Spain, 29010

Hospital Clinico Universitario de Valencia; Servicio de Neurologia

Valencia, Spain, 46010

Sweden

Sahlgrenska Sjukhuset; Neurology

Göteborg, Sweden, 413 45

Karolinska Universitetssjukhuset Solna Neurology

Stockholm, Sweden, 113 41

Karolinska Universitetssjukhuset Huddinge

Stockholm, Sweden, 171 64

Norrlands Universitetssjukhus

Umeå, Sweden, 901 85

Turkey

Hacettepe University Medical Faculty; Neurology

Ankara, Turkey, 06100

Haseki Training and Research Hospital

Istanbul, Turkey, 34096

Istanbul Universitesi - Cerrahpasa Cerrahpasa Tip Fakultesi; Noroloji Anabilim Dali

Istanbul, Turkey, 34098

Istanbul Bilim Universty Medical Fac.

Istanbul, Turkey, 34394

Ege University Medical Faculty

Izmir, Turkey, 35100

Kocaeli University Medical Faculty

Kocaeli, Turkey, 41380

Ondokuz Mayis Univ. Med. Fac.; Neurology

Samsun, Turkey, 55139

Karadeniz Tecnical Uni. Med. Fac.; Neurology

Trabzon, Turkey, 61080

Ukraine

Mun.Med.Proph.Inst.?Chernihiv Reg.Hosp.?; Neurology Department

Chernihiv, Ukraine, 14029

City Clinical Hospital #4

Dnipropetrovsk, Ukraine, 49102

State Institution V.K. Gusak Institute of Urgent and Recover; Dep of Reconstructive Angioneurology a

Donetsk, Ukraine, 83045

Road Clinical Hospital of Donetsk Station; Neurology Department

Donetsk, Ukraine, 83114

Regional Clinical Hospital; Neurology Department

Ivano-Frankivsk, Ukraine, 76008

United Kingdom

Royal Devon and Exeter Hospital (Wonford)

Exeter, United Kingdom, EX2 5DW

Kings College Hospital; Neurosciences Clinical Trials Office

London, United Kingdom, SE5 9NT

City General Hospital; Department of Neurology

Stoke on Trent, United Kingdom, ST4 6QG

Morriston Hospital

Swansea, United Kingdom, SA6 6NL

Sponsors and Collaborators

Hoffmann-La Roche

Investigators

• Study Director: Clinical Trials; Hoffmann-La Roche

More Information

Publications automatically indexed to this study by ClinicalTrials.gov Identifier (NCT Number):

Arnold DL, Sprenger T, Bar-Or A, Wolinsky JS, Kappos L, Kolind S, Bonati U, Magon S, van Beek J, Koendgen H, Bortolami O, Bernasconi C, Gaetano L, Traboulsee A. Ocrelizumab reduces thalamic volume loss in patients with RMS and PPMS. Mult Scler. 2022 Oct;28(12):1927-1936. doi: 10.1177/13524585221097561. Epub 2022 Jun 7.

Krishnan AP, Song Z, Clayton D, Gaetano L, Jia X, de Crespigny A, Bengtsson T, Carano RAD. Joint MRI T1 Unenhancing and Contrast-enhancing Multiple Sclerosis Lesion Segmentation with Deep Learning in OPERA Trials. Radiology. 2022 Mar;302(3):662-673. doi: 10.1148/radiol.211528. Epub 2021 Dec 14.

Giovannoni G, Kappos L, de Seze J, Hauser SL, Overell J, Koendgen H, Manfrini M, Wang Q, Wolinsky JS. Risk of requiring a walking aid after 6.5 years of ocrelizumab treatment in patients with relapsing multiple sclerosis: Data from the OPERA I and OPERA II trials. Eur J Neurol. 2022 Apr;29(4):1238-1242. doi: 10.1111/ene.14823. Epub 2021 May 5.

Hauser SL, Kappos L, Arnold DL, Bar-Or A, Brochet B, Naismith RT, Traboulsee A, Wolinsky JS, Belachew S, Koendgen H, Levesque V, Manfrini M, Model F, Hubeaux S, Mehta L, Montalban X. Five years of ocrelizumab in relapsing multiple sclerosis: OPERA studies open-label extension. Neurology. 2020 Sep 29;95(13):e1854-e1867. doi: 10.1212/WNL.0000000000010376. Epub 2020 Jul 20.

Kappos L, Wolinsky JS, Giovannoni G, Arnold DL, Wang Q, Bernasconi C, Model F, Koendgen H, Manfrini M, Belachew S, Hauser SL. Contribution of Relapse-Independent Progression vs Relapse-Associated Worsening to Overall Confirmed Disability Accumulation in Typical Relapsing Multiple Sclerosis in a Pooled Analysis of 2 Randomized Clinical Trials. JAMA Neurol. 2020 Sep 1;77(9):1132-1140. doi: 10.1001/jamaneurol.2020.1568.

Hauser SL, Bar-Or A, Comi G, Giovannoni G, Hartung HP, Hemmer B, Lublin F, Montalban X, Rammohan KW, Selmaj K, Traboulsee A, Wolinsky JS, Arnold DL, Klingelschmitt G, Masterman D, Fontoura P, Belachew S, Chin P, Mairon N, Garren H, Kappos L; OPERA I and OPERA II Clinical Investigators. Ocrelizumab versus Interferon Beta-1a in Relapsing Multiple Sclerosis. N Engl J Med. 2017 Jan 19;376(3):221-234. doi: 10.1056/NEJMoa1601277. Epub 2016 Dec 21.

• Responsible Party: Hoffmann-La Roche
• ClinicalTrials.gov Identifier: NCT01412333
• Other Study ID Numbers: WA21093; 2010-020315-36 ( EudraCT Number )
• First Posted: August 9, 2011
• Results First Posted: July 18, 2017
• Last Update Posted: March 3, 2023
• Last Verified: March 2023

Additional relevant MeSH terms:

Ocrelizumab; Multiple Sclerosis; Sclerosis; Pathologic Processes; Demyelinating Autoimmune Diseases, CNS; Autoimmune Diseases of the Nervous System; Nervous System Diseases; Demyelinating Diseases; Autoimmune Diseases; Immune System Diseases; Interferons; Interferon-beta; Interferon beta-1a; Antineoplastic Agents; Antiviral Agents; Anti-Infective Agents; Immunologic Factors; Physiological Effects of Drugs; Adjuvants, Immunologic