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Rituximab vs Ocrelizumab in Relapsing-Remitting Multiple Sclerosis.
Roos, Izanne; Hughes, Stella; McDonnell, Gavin; Malpas, Charles B; Sharmin, Sifat; Boz, Cavit; Alroughani, Raed; Ozakbas, Serkan; Buzzard, Katherine; Skibina, Olga; van der Walt, Anneke; Butzkueven, Helmut; Lechner-Scott, Jeannette; Kuhle, Jens; Terzi, Murat; Laureys, Guy; Van Hijfte, Liesbeth; John, Nevin; Grammond, Pierre; Grand'Maison, Francois; Soysal, Aysun; Jensen, Ana Voldsgaard; Rasmussen, Peter Vestergaard; Svendsen, Kristina Bacher; Barzinji, Ismael; Nielsen, Helle Hvilsted; Sejbæk, Tobias; Prakash, Sivagini; Stilund, Morten Leif Munding; Weglewski, Arkadiusz; Issa, Nadia Mubder; Kant, Matthias; Sellebjerg, Finn; Gray, Orla; Magyari, Melinda; Kalincik, Tomas.
Affiliation
  • Roos I; Neuroimmunology Centre, Royal Melbourne Hospital, Melbourne, Victoria, Australia.
  • Hughes S; CORe, Department of Medicine, University of Melbourne, Melbourne, Victoria, Australia.
  • McDonnell G; Royal Victoria Hospital, Belfast, United Kingdom.
  • Malpas CB; Belfast City Hospital, Belfast, United Kingdom.
  • Sharmin S; Neuroimmunology Centre, Royal Melbourne Hospital, Melbourne, Victoria, Australia.
  • Boz C; CORe, Department of Medicine, University of Melbourne, Melbourne, Victoria, Australia.
  • Alroughani R; CORe, Department of Medicine, University of Melbourne, Melbourne, Victoria, Australia.
  • Ozakbas S; KTU Medical Faculty Farabi Hospital, Trabzon, Turkey.
  • Buzzard K; Division of Neurology, Department of Medicine, Amiri Hospital, Sharq, Kuwait.
  • Skibina O; Dokuz Eylul University, Konak/Izmir, Turkey.
  • van der Walt A; Neuroimmunology Centre, Royal Melbourne Hospital, Melbourne, Victoria, Australia.
  • Butzkueven H; Department of Neurology, Box Hill Hospital, Melbourne, Victoria, Australia.
  • Lechner-Scott J; Monash University, Melbourne, Victoria, Australia.
  • Kuhle J; Department of Neurology, Box Hill Hospital, Melbourne, Victoria, Australia.
  • Terzi M; Monash University, Melbourne, Victoria, Australia.
  • Laureys G; Department of Neurology, The Alfred Hospital, Melbourne, Victoria, Australia.
  • Van Hijfte L; Department of Neurology, The Alfred Hospital, Melbourne, Victoria, Australia.
  • John N; Department of Neuroscience, Central Clinical School, Monash University, Melbourne, Victoria, Australia.
  • Grammond P; Department of Neurology, The Alfred Hospital, Melbourne, Victoria, Australia.
  • Grand'Maison F; Department of Neuroscience, Central Clinical School, Monash University, Melbourne, Victoria, Australia.
  • Soysal A; School of Medicine and Public Health, University Newcastle, Newcastle, New South Wales, Australia.
  • Jensen AV; Department of Neurology, John Hunter Hospital, Hunter New England Health, Newcastle, New South Wales, Australia.
  • Rasmussen PV; Departments of Medicine, Biomedicine, and Clinical Research, Neurologic Clinic and Policlinic, University Hospital and University of Basel, Basel, Switzerland.
  • Svendsen KB; Medical Faculty, 19 Mayis University, Samsun, Turkey.
  • Barzinji I; Department of Neurology, Ghent University Hospital, Ghent, Belgium.
  • Nielsen HH; Department of Neurology, Ghent University Hospital, Ghent, Belgium.
  • Sejbæk T; Department of Neurology, Monash Health, Melbourne, Victoria, Australia.
  • Prakash S; Department of Medicine, School of Clinical Sciences, Monash University, Melbourne, Victoria, Australia.
  • Stilund MLM; CISSS Chaudière-Appalache, Levis, Canada.
  • Weglewski A; Neuro Rive-Sud, Longueuil, Québec, Canada.
  • Issa NM; Bakirkoy Education and Research Hospital for Psychiatric and Neurological Diseases, Istanbul, Turkey.
  • Kant M; Danish Multiple Sclerosis Center, Rigshospitalet Glostrup, Copenhagen University Hospital, Denmark.
  • Sellebjerg F; Department of Neurology, Aarhus University Hospital, Aarhus, Denmark.
  • Gray O; Department of Neurology, Aarhus University Hospital, Aarhus, Denmark.
  • Magyari M; Aalborg University Hospital, Denmark.
  • Kalincik T; The Multiple Sclerosis Clinic, Department of Neurology, Odense University Hospital, Odense C, Denmark.
JAMA Neurol ; 80(8): 789-797, 2023 08 01.
Article in En | MEDLINE | ID: mdl-37307006
ABSTRACT
Importance Ocrelizumab, a humanized monoclonal antibody targeted against CD20+ B cells, reduces the frequency of relapses by 46% and disability worsening by 40% compared with interferon beta 1a in relapsing-remitting multiple sclerosis (MS). Rituximab, a chimeric monoclonal anti-CD20 agent, is often prescribed as an off-label alternative to ocrelizumab.

Objective:

To evaluate whether the effectiveness of rituximab is noninferior to ocrelizumab in relapsing-remitting MS. Design, Setting, and

Participants:

This was an observational cohort study conducted between January 2015 and March 2021. Patients were included in the treatment group for the duration of study therapy and were recruited from the MSBase registry and Danish MS Registry (DMSR). Included patients had a history of relapsing-remitting MS treated with ocrelizumab or rituximab, a minimum 6 months of follow-up, and sufficient data to calculate the propensity score. Patients with comparable baseline characteristics were 16 matched with propensity score on age, sex, MS duration, disability (Expanded Disability Status Scale), prior relapse rate, prior therapy, disease activity (relapses, disability accumulation, or both), magnetic resonance imaging lesion burden (missing values imputed), and country. Exposure Treatment with ocrelizumab or rituximab after 2015. Main outcomes and

Measures:

Noninferiority comparison of annualized rate of relapses (ARRs), with a prespecified noninferiority margin of 1.63 rate ratio. Secondary end points were relapse and 6-month confirmed disability accumulation in pairwise-censored groups.

Results:

Of the 6027 patients with MS who were treated with ocrelizumab or rituximab, a total of 1613 (mean [SD] age; 42.0 [10.8] years; 1089 female [68%]) fulfilled the inclusion criteria and were included in the analysis (898 MSBase, 715 DMSR). A total of 710 patients treated with ocrelizumab (414 MSBase, 296 DMSR) were matched with 186 patients treated with rituximab (110 MSBase, 76 DMSR). Over a pairwise censored mean (SD) follow-up of 1.4 (0.7) years, the ARR ratio was higher in patients treated with rituximab than in those treated with ocrelizumab (rate ratio, 1.8; 95% CI, 1.4-2.4; ARR, 0.20 vs 0.09; P < .001). The cumulative hazard of relapses was higher among patients treated with rituximab than those treated with ocrelizumab (hazard ratio, 2.1; 95% CI, 1.5-3.0). No difference in the risk of disability accumulation was observed between groups. Results were confirmed in sensitivity analyses.

Conclusion:

In this noninferiority comparative effectiveness observational cohort study, results did not show noninferiority of treatment with rituximab compared with ocrelizumab. As administered in everyday practice, rituximab was associated with a higher risk of relapses than ocrelizumab. The efficacy of rituximab and ocrelizumab administered at uniform doses and intervals is being further evaluated in randomized noninferiority clinical trials.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Multiple Sclerosis, Relapsing-Remitting / Multiple Sclerosis Type of study: Clinical_trials / Etiology_studies / Incidence_studies / Observational_studies / Risk_factors_studies Limits: Female / Humans Language: En Journal: JAMA Neurol Year: 2023 Type: Article Affiliation country: Australia
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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Multiple Sclerosis, Relapsing-Remitting / Multiple Sclerosis Type of study: Clinical_trials / Etiology_studies / Incidence_studies / Observational_studies / Risk_factors_studies Limits: Female / Humans Language: En Journal: JAMA Neurol Year: 2023 Type: Article Affiliation country: Australia