Comparison Between Dimethyl Fumarate, Fingolimod, and Ocrelizumab After Natalizumab Cessation

Chao Zhu; Tomas Kalincik; Dana Horakova; Zhen Zhou; Katherine Buzzard; Olga Skibina; Raed Alroughani; Guillermo Izquierdo; Sara Eichau; Jens Kuhle; Francesco Patti; Francois Grand'Maison; Suzanne Hodgkinson; Pierre Grammond; Jeannette Lechner-Scott; Ernest Butler; Alexandre Prat; Marc Girard; Pierre Duquette; Richard A L Macdonell; Bianca Weinstock-Guttman; Serkan Ozakbas; Mark Slee; Maria Jose Sa; Vincent Van Pesch; Michael Barnett; Bart Van Wijmeersch; Oliver Gerlach; Julie Prevost; Murat Terzi; Cavit Boz; Guy Laureys; Liesbeth Van Hijfte; Allan G Kermode; Justin Garber; Bassem Yamout; Samia J Khoury; Daniel Merlo; Mastura Monif; Vilija Jokubaitis; Anneke van der Walt; Helmut Butzkueven; MSBase Study Group

doi:10.1001/jamaneurol.2023.1542

Comparison Between Dimethyl Fumarate, Fingolimod, and Ocrelizumab After Natalizumab Cessation

JAMA Neurol. 2023 Jul 1;80(7):739-748. doi: 10.1001/jamaneurol.2023.1542.

Authors

Chao Zhu¹, Tomas Kalincik^{2

3}, Dana Horakova⁴, Zhen Zhou⁵, Katherine Buzzard^{1

6}, Olga Skibina^{1

6

7}, Raed Alroughani⁸, Guillermo Izquierdo⁹, Sara Eichau⁹, Jens Kuhle¹⁰, Francesco Patti¹¹, Francois Grand'Maison¹², Suzanne Hodgkinson¹³, Pierre Grammond¹⁴, Jeannette Lechner-Scott¹⁵, Ernest Butler¹⁶, Alexandre Prat¹⁷, Marc Girard¹⁷, Pierre Duquette¹⁷, Richard A L Macdonell¹⁸, Bianca Weinstock-Guttman¹⁹, Serkan Ozakbas²⁰, Mark Slee²¹, Maria Jose Sa²², Vincent Van Pesch²³, Michael Barnett²⁴, Bart Van Wijmeersch²⁵, Oliver Gerlach²⁶, Julie Prevost²⁷, Murat Terzi²⁸, Cavit Boz²⁹, Guy Laureys³⁰, Liesbeth Van Hijfte³⁰, Allan G Kermode³¹, Justin Garber³², Bassem Yamout³³, Samia J Khoury³³, Daniel Merlo¹, Mastura Monif^{1

7}, Vilija Jokubaitis¹, Anneke van der Walt^{1

7}, Helmut Butzkueven^{1

7}; MSBase Study Group

Collaborators

MSBase Study Group:
Thomas P Leist, Lily Habib, Paarami Udugama, Orla Gray, Dana Horakova, Charlotte Sartori, Rein More, Ana Siddiqui, Pamela Farr, Dusko Stupar, Cynthia Tang, Alison Le, Sonya Smirnova, Gaurang Palshetkar, Tim Spelman

Affiliations

¹ Department of Neuroscience, Central Clinical School, Monash University, Melbourne, Victoria, Australia.
² Clinical Outcomes Research Unit (CORe), Department of Medicine, University of Melbourne, Melbourne, Victoria, Australia.
³ Department of Neurology, Royal Melbourne Hospital, Melbourne, Victoria, Australia.
⁴ Charles University in Prague and General University Hospital, Prague, Czech Republic.
⁵ School of Public Health and Preventive Medicine, Monash University, Melbourne, Victoria, Australia.
⁶ Department of Neurology, Box Hill Hospital, Melbourne, Victoria, Australia.
⁷ Department of Neurology, Alfred Hospital, Melbourne, Victoria, Australia.
⁸ Amiri Hospital, Sharq, Kuwait.
⁹ Hospital Universitario Virgen Macarena, Sevilla, Spain.
¹⁰ University Hospital and University of Basel, Basel, Switzerland.
¹¹ Multiple Sclerosis Center, University of Catania, Catania, Italy.
¹² Neuro Rive-Sud, Longueuil, Québec, Canada.
¹³ Liverpool Hospital, Sydney, New South Wales, Australia.
¹⁴ CISSS Chaudière-Appalache, Levis, Québec, Canada.
¹⁵ University Newcastle, Newcastle, New South Wales, Australia.
¹⁶ Monash Medical Centre, Melbourne, Victoria, Australia.
¹⁷ CHUM MS Center and Université de Montréal, Montréal, Québec, Canada.
¹⁸ Austin Health, Melbourne, Victoria, Australia.
¹⁹ Buffalo General Medical Center, Buffalo, New York.
²⁰ Dokuz Eylul University, Konak/Izmir, Turkey.
²¹ Flinders University, Adelaide, South Australia, Australia.
²² Centro Hospitalar Universitario de São João, Porto, Portugal.
²³ Cliniques Universitaires Saint-Luc, Brussels, Belgium.
²⁴ Brain and Mind Centre, Sydney, New South Wales, Australia.
²⁵ Rehabilitation and MS-Centre Overpelt and Hasselt University, Hasselt, Belgium.
²⁶ Zuyderland Medical Center, Sittard-Geleen, the Netherlands.
²⁷ CSSS Saint-Jérôme, Saint-Jerome, Québec, Canada.
²⁸ 19 Mayis University, Samsun, Turkey.
²⁹ KTU Medical Faculty Farabi Hospital, Trabzon, Turkey.
³⁰ Universitary Hospital Ghent, Ghent, Belgium.
³¹ University of Western Australia, Nedlands, Western Australia, Australia.
³² Westmead Hospital, Sydney, New South Wales, Australia.
³³ American University of Beirut Medical Center, Beirut, Lebanon.

PMID: 37273217
PMCID: PMC10242509 (available on 2024-06-05)
DOI: 10.1001/jamaneurol.2023.1542

Abstract

Importance: Natalizumab cessation is associated with a risk of rebound disease activity. It is important to identify the optimal switch disease-modifying therapy strategy after natalizumab to limit the risk of severe relapses.

Objectives: To compare the effectiveness and persistence of dimethyl fumarate, fingolimod, and ocrelizumab among patients with relapsing-remitting multiple sclerosis (RRMS) who discontinued natalizumab.

Design, setting, and participants: In this observational cohort study, patient data were collected from the MSBase registry between June 15, 2010, and July 6, 2021. The median follow-up was 2.7 years. This was a multicenter study that included patients with RRMS who had used natalizumab for 6 months or longer and then were switched to dimethyl fumarate, fingolimod, or ocrelizumab within 3 months after natalizumab discontinuation. Patients without baseline data were excluded from the analysis. Data were analyzed from May 24, 2022, to January 9, 2023.

Exposures: Dimethyl fumarate, fingolimod, and ocrelizumab.

Main outcomes and measures: Primary outcomes were annualized relapse rate (ARR) and time to first relapse. Secondary outcomes were confirmed disability accumulation, disability improvement, and subsequent treatment discontinuation, with the comparisons for the first 2 limited to fingolimod and ocrelizumab due to the small number of patients taking dimethyl fumarate. The associations were analyzed after balancing covariates using an inverse probability of treatment weighting method.

Results: Among 66 840 patients with RRMS, 1744 had used natalizumab for 6 months or longer and were switched to dimethyl fumarate, fingolimod, or ocrelizumab within 3 months of natalizumab discontinuation. After excluding 358 patients without baseline data, a total of 1386 patients (mean [SD] age, 41.3 [10.6] years; 990 female [71%]) switched to dimethyl fumarate (138 [9.9%]), fingolimod (823 [59.4%]), or ocrelizumab (425 [30.7%]) after natalizumab. The ARR for each medication was as follows: ocrelizumab, 0.06 (95% CI, 0.04-0.08); fingolimod, 0.26 (95% CI, 0.12-0.48); and dimethyl fumarate, 0.27 (95% CI, 0.12-0.56). The ARR ratio of fingolimod to ocrelizumab was 4.33 (95% CI, 3.12-6.01) and of dimethyl fumarate to ocrelizumab was 4.50 (95% CI, 2.89-7.03). Compared with ocrelizumab, the hazard ratio (HR) of time to first relapse was 4.02 (95% CI, 2.83-5.70) for fingolimod and 3.70 (95% CI, 2.35-5.84) for dimethyl fumarate. The HR of treatment discontinuation was 2.57 (95% CI, 1.74-3.80) for fingolimod and 4.26 (95% CI, 2.65-6.84) for dimethyl fumarate. Fingolimod use was associated with a 49% higher risk for disability accumulation compared with ocrelizumab. There was no significant difference in disability improvement rates between fingolimod and ocrelizumab.

Conclusion and relevance: Study results show that among patients with RRMS who switched from natalizumab to dimethyl fumarate, fingolimod, or ocrelizumab, ocrelizumab use was associated with the lowest ARR and discontinuation rates, and the longest time to first relapse.

Publication types

Observational Study
Multicenter Study

MeSH terms

Adult
Dimethyl Fumarate / adverse effects
Female
Fingolimod Hydrochloride* / therapeutic use
Humans
Immunologic Factors / adverse effects
Immunosuppressive Agents / adverse effects
Multiple Sclerosis, Relapsing-Remitting* / drug therapy
Natalizumab / adverse effects
Neoplasm Recurrence, Local / drug therapy
Recurrence

Substances

Fingolimod Hydrochloride
Natalizumab
Dimethyl Fumarate
ocrelizumab
Immunosuppressive Agents
Immunologic Factors