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    Switch to Natalizumab versus Fingolimod in Active Relapsing-Remitting Multiple Sclerosis

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    Kalincik Ann Neurol 2014.doc (113Kb)

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    Author
    Kalincik, T; Horakova, D; Spelman, T; Jokubaitis, V; Trojano, M; Lugaresi, A; Izquierdo, G; Rozsa, C; Grammond, P; Alroughani, R; ...
    Date
    2015-03-01
    Source Title
    ANNALS OF NEUROLOGY
    Publisher
    WILEY
    University of Melbourne Author/s
    Kalincik, Tomas; Butzkueven, Helmut; Jokubaitis, Vilija; Spelman, Timothy
    Affiliation
    Medicine - Royal Melbourne Hospital
    Metadata
    Show full item record
    Document Type
    Journal Article
    Citations
    Kalincik, T; Horakova, D; Spelman, T; Jokubaitis, V; Trojano, M; Lugaresi, A; Izquierdo, G; Rozsa, C; Grammond, P; Alroughani, R; Duquette, P; Girard, M; Pucci, E; Lechner-Scott, J; Slee, M; Fernandez-Bolanos, R; Grand'Maison, F; Hupperts, R; Verheul, F; Hodgkinson, S; Oreja-Guevara, C; Spitaleri, D; Barnett, M; Terzi, M; Bergamaschi, R; McCombe, P; Sanchez-Menoyo, J; Simo, M; Csepany, T; Rum, G; Boz, C; Havrdova, E; Butzkueven, H, Switch to Natalizumab versus Fingolimod in Active Relapsing-Remitting Multiple Sclerosis, ANNALS OF NEUROLOGY, 2015, 77 (3), pp. 425 - 435
    Access Status
    Open Access
    URI
    http://hdl.handle.net/11343/45130
    DOI
    10.1002/ana.24339
    NHMRC Grant code
    NHMRC/1083539
    NHMRC/1071124
    NHMRC/1129189
    NHMRC/1140766
    Abstract
    OBJECTIVE: In patients suffering multiple sclerosis activity despite treatment with interferon β or glatiramer acetate, clinicians often switch therapy to either natalizumab or fingolimod. However, no studies have directly compared the outcomes of switching to either of these agents. METHODS: Using MSBase, a large international, observational, prospectively acquired cohort study, we identified patients with relapsing-remitting multiple sclerosis experiencing relapses or disability progression within the 6 months immediately preceding switch to either natalizumab or fingolimod. Quasi-randomization with propensity score-based matching was used to select subpopulations with comparable baseline characteristics. Relapse and disability outcomes were compared in paired, pairwise-censored analyses. RESULTS: Of the 792 included patients, 578 patients were matched (natalizumab, n = 407; fingolimod, n = 171). Mean on-study follow-up was 12 months. The annualized relapse rates decreased from 1.5 to 0.2 on natalizumab and from 1.3 to 0.4 on fingolimod, with 50% relative postswitch difference in relapse hazard (p = 0.002). A 2.8 times higher rate of sustained disability regression was observed after the switch to natalizumab in comparison to fingolimod (p < 0.001). No difference in the rate of sustained disability progression events was observed between the groups. The change in overall disability burden (quantified as area under the disability-time curve) differed between natalizumab and fingolimod (-0.12 vs 0.04 per year, respectively, p < 0.001). INTERPRETATION: This study suggests that in active multiple sclerosis during treatment with injectable disease-modifying therapies, switching to natalizumab is more effective than switching to fingolimod in reducing relapse rate and short-term disability burden.

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