Association of Initial Disease-Modifying Therapy with Later Conversion to Secondary Progressive Multiple Sclerosis

Brown, J.W.L.; Coles, A.; Horáková, D.; Kubala Havrdová, E.; Izquierdo, G.; Prat, A.; Girard, M.

doi:10.1001/jama.2018.20588

Publication:
Association of Initial Disease-Modifying Therapy with Later Conversion to Secondary Progressive Multiple Sclerosis

dc.authorscopusid	56334822000
dc.authorscopusid	7005609267
dc.authorscopusid	55053678000
dc.authorscopusid	57201596736
dc.authorscopusid	7005179252
dc.authorscopusid	7103277065
dc.authorscopusid	8365701900
dc.contributor.author	Brown, J.W.L.
dc.contributor.author	Coles, A.
dc.contributor.author	Horáková, D.
dc.contributor.author	Kubala Havrdová, E.
dc.contributor.author	Izquierdo, G.
dc.contributor.author	Prat, A.
dc.contributor.author	Girard, M.
dc.date.accessioned	2020-06-21T13:04:54Z
dc.date.available	2020-06-21T13:04:54Z
dc.date.issued	2019
dc.department	Ondokuz Mayıs Üniversitesi	en_US
dc.department-temp	[Brown] William Langdon, Department of Clinical Neurosciences, University of Cambridge, Cambridge, Cambridgeshire, United Kingdom, UCL Queen Square Institute of Neurology, London, United Kingdom, Melbourne Brain Centre, University of Melbourne, Melbourne, VIC, Australia; [Coles] Alasdair John, Department of Clinical Neurosciences, University of Cambridge, Cambridge, Cambridgeshire, United Kingdom; [Horáková] Dana, Department of Neurology, Všeobecná Fakultní Nemocnice v Praze, Prague, Czech Republic, Charles University, Prague, Czech Republic; [Kubala Havrdová] Eva Kubala, Department of Neurology, Všeobecná Fakultní Nemocnice v Praze, Prague, Czech Republic, Charles University, Prague, Czech Republic; [Izquierdo] Guillermo Ayuso, Hospital Universitario Virgen Macarena, Sevilla, Spain; [Prat] Alexandre, Hôpital Notre-Dame, Montreal, QC, Canada, University of Montreal, Montreal, QC, Canada; [Girard] Marc, Hôpital Notre-Dame, Montreal, QC, Canada, University of Montreal, Montreal, QC, Canada; [Duquette] Pierre Pascal, Hôpital Notre-Dame, Montreal, QC, Canada, University of Montreal, Montreal, QC, Canada; [Trojano] Maria, Department of Basic Medical Sciences, Università degli studi di Bari Aldo Moro, Bari, BA, Italy; [Lugaresi] Alessandra, Department of Neuroscience, Imaging and Clinical Sciences, University of G. d'Annunzio Chieti and Pescara, Chieti, CH, Italy; [Bergamaschi] Roberto, IRCCS Fondazione Mondino, Pavia, PV, Italy; [Grammond] Pierre, CISSS chaudi'Re-Appalache, Centre-Hospitalier, Levis, Canada; [Alroughani] Raed A., Al-Amiri Hospital, Safat, Kuwait; [Hupperts] Raymond M.M., Zuyderland, Sittard-Geleen, Limburg, Netherlands; [McCombe] Pamela A., The University of Queensland, Brisbane, QLD, Australia; [van Pesch] Vincent, Cliniques Universitaires Saint-Luc, Brussels, BRU, Belgium; [Sola] Patrizia, Department of Neuroscience, Azienda Ospedaliera Universitaria, Modena, Italy; [Ferraro] Diana, Department of Neuroscience, Azienda Ospedaliera Universitaria, Modena, Italy; [Grand'Maison] François, Neuro Rive-Sud, Quebec, QC, Canada; [Terzi] Murat, Faculty of Medicine, Ondokuz Mayis Üniversitesi, Samsun, Turkey; [Lechner-Scott] Jeannette S., School of Medicine and Public Health, Callaghan, NSW, Australia, Department of Neurology, John Hunter Hospital, Newcastle, NSW, Australia; [Flechter] Schlomo, Shamir Medical Center, Beer Yacov, Israel; [Slee] Mark, Flinders University, Adelaide, SA, Australia; [Shaygannejad] Vahid, Isfahan University of Medical Sciences, Isfahan, Isfahan, Iran; [Pucci] Eugenio, UOC Neurologia, Macerata, Italy; [Granella] Franco, Università di Parma, Parma, PR, Italy; [Jokubaitis] Vilija G., Department of Medicine, Melbourne, VIC, Australia, Department of Neurology, Royal Melbourne Hospital, Melbourne, VIC, Australia; [Willis] Mark Douglas, Department of Neurology, Cardiff University, Cardiff, South Glamorgan, Wales, United Kingdom; [Rice] Claire M., University of Bristol, Bristol, United Kingdom; [Scolding] Neil J., University of Bristol, Bristol, United Kingdom; [Wilkins] Alistair L., University of Bristol, Bristol, United Kingdom; [Pearson] Owen Rhys, Swansea Bay University Health Board, Port Talbot, West Glamorgan, Wales, United Kingdom; [Ziemssen] Tjalf, Department of Neurology, MS Center Dresden, Dresden, Germany; [Hutchinson] Michael K., St Vincent's University Hospital, Dublin, Leinster, Ireland; [Harding] Katharine Elizabeth, Division of Psychological Medicine and Clinical Neurosciences, Cardiff University, Cardiff, South Glamorgan, Wales, United Kingdom; [Jones] Joanne Louise, Department of Clinical Neurosciences, University of Cambridge, Cambridge, Cambridgeshire, United Kingdom; [McGuigan] Christopher, St Vincent's University Hospital, Dublin, Leinster, Ireland; [Butzkueven] Helmut, Department of Medicine, Melbourne, VIC, Australia, Department of Neurology, Royal Melbourne Hospital, Melbourne, VIC, Australia, Department of Neurology, Monash University, Melbourne, VIC, Australia; [Kalincik] Tomas, Melbourne Brain Centre, University of Melbourne, Melbourne, VIC, Australia, Department of Medicine, Melbourne, VIC, Australia, Department of Neurology, Royal Melbourne Hospital, Melbourne, VIC, Australia; [Robertson] Neil P., Division of Psychological Medicine and Clinical Neurosciences, Cardiff University, Cardiff, South Glamorgan, Wales, United Kingdom	en_US
dc.description.abstract	Importance: Within 2 decades of onset, 80% of untreated patients with relapsing-remitting multiple sclerosis (MS) convert to a phase of irreversible disability accrual termed secondary progressive MS. The association between disease-modifying treatments (DMTs), and this conversion has rarely been studied and never using a validated definition. Objective: To determine the association between the use, the type of, and the timing of DMTs with the risk of conversion to secondary progressive MS diagnosed with a validated definition. Design, Setting, and Participants: Cohort study with prospective data from 68 neurology centers in 21 countries examining patients with relapsing-remitting MS commencing DMTs (or clinical monitoring) between 1988-2012 with minimum 4 years' follow-up. Exposures: The use, type, and timing of the following DMTs: interferon beta, glatiramer acetate, fingolimod, natalizumab, or alemtuzumab. After propensity-score matching, 1555 patients were included (last follow-up, February 14, 2017). Main Outcome and Measure: Conversion to objectively defined secondary progressive MS. Results: Of the 1555 patients, 1123 were female (mean baseline age, 35 years [SD, 10]). Patients initially treated with glatiramer acetate or interferon beta had a lower hazard of conversion to secondary progressive MS than matched untreated patients (HR, 0.71; 95% CI, 0.61-0.81; P <.001; 5-year absolute risk, 12% [49 of 407] vs 27% [58 of 213]; median follow-up, 7.6 years [IQR, 5.8-9.6]), as did fingolimod (HR, 0.37; 95% CI, 0.22-0.62; P <.001; 5-year absolute risk, 7% [6 of 85] vs 32% [56 of 174]; median follow-up, 4.5 years [IQR, 4.3-5.1]); natalizumab (HR, 0.61; 95% CI, 0.43-0.86; P =.005; 5-year absolute risk, 19% [16 of 82] vs 38% [62 of 164]; median follow-up, 4.9 years [IQR, 4.4-5.8]); and alemtuzumab (HR, 0.52; 95% CI, 0.32-0.85; P =.009; 5-year absolute risk, 10% [4 of 44] vs 25% [23 of 92]; median follow-up, 7.4 years [IQR, 6.0-8.6]). Initial treatment with fingolimod, alemtuzumab, or natalizumab was associated with a lower risk of conversion than initial treatment with glatiramer acetate or interferon beta (HR, 0.66; 95% CI, 0.44-0.99; P =.046); 5-year absolute risk, 7% [16 of 235] vs 12% [46 of 380]; median follow-up, 5.8 years [IQR, 4.7-8.0]). The probability of conversion was lower when glatiramer acetate or interferon beta was started within 5 years of disease onset vs later (HR, 0.77; 95% CI, 0.61-0.98; P =.03; 5-year absolute risk, 3% [4 of 120] vs 6% [2 of 38]; median follow-up, 13.4 years [IQR, 11-18.1]). When glatiramer acetate or interferon beta were escalated to fingolimod, alemtuzumab, or natalizumab within 5 years vs later, the HR was 0.76 (95% CI, 0.66-0.88; P <.001; 5-year absolute risk, 8% [25 of 307] vs 14% [46 of 331], median follow-up, 5.3 years [IQR], 4.6-6.1). Conclusions and Relevance: Among patients with relapsing-remitting MS, initial treatment with fingolimod, alemtuzumab, or natalizumab was associated with a lower risk of conversion to secondary progressive MS vs initial treatment with glatiramer acetate or interferon beta. These findings, considered along with these therapies' risks, may help inform decisions about DMT selection. © 2019 American Medical Association. All rights reserved.	en_US
dc.identifier.doi	10.1001/jama.2018.20588
dc.identifier.endpage	187	en_US
dc.identifier.issn	0098-7484
dc.identifier.issn	1538-3598
dc.identifier.issue	2	en_US
dc.identifier.pmid	30644981
dc.identifier.scopus	2-s2.0-85059962064
dc.identifier.scopusquality	Q1
dc.identifier.startpage	175	en_US
dc.identifier.uri	https://doi.org/10.1001/jama.2018.20588
dc.identifier.volume	321	en_US
dc.identifier.wos	WOS:000455606300016
dc.identifier.wosquality	Q1
dc.language.iso	en	en_US
dc.publisher	American Medical Association smcleod@itsa.ucsf.edu	en_US
dc.relation.ispartof	JAMA-Journal of the American Medical Association	en_US
dc.relation.journal	Jama-Journal of the American Medical Association	en_US
dc.relation.publicationcategory	Makale - Uluslararası Hakemli Dergi - Kurum Öğretim Elemanı	en_US
dc.rights	info:eu-repo/semantics/openAccess	en_US
dc.title	Association of Initial Disease-Modifying Therapy with Later Conversion to Secondary Progressive Multiple Sclerosis	en_US
dc.type	Article	en_US
dspace.entity.type	Publication

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Association of Initial Disease-Modifying Therapy with Later Conversion to Secondary Progressive Multiple Sclerosis