Efficacy and Safety of Masitinib in Progressive Forms of Multiple Sclerosis: A Randomized, Phase 3, Clinical Trial

Patrick Vermersch; Luis Brieva-Ruiz; Robert J Fox; Friedemann Paul; Lluis Ramio-Torrenta; Matthias Schwab; Alain Moussy; Colin Mansfield; Olivier Hermine; Maciej Maciejowski; AB07002 Study Group

doi:10.1212/NXI.0000000000001148

Efficacy and Safety of Masitinib in Progressive Forms of Multiple Sclerosis: A Randomized, Phase 3, Clinical Trial

Neurol Neuroimmunol Neuroinflamm. 2022 Feb 21;9(3):e1148. doi: 10.1212/NXI.0000000000001148. Print 2022 May.

Collaborators

AB07002 Study Group:
N Hecham, N Haydeé Deri, J Djelilovic-Vranic, I Milanov, P Shotekov, G Blevins, J Girard, Y Lapierre, W Camu, G Castelnovo, P Clavelou, P Hautecoeur, M Marziniak, C Mayer, P Oschmann, G Reifschneider, I Schoell, B Tackenberg, F Then Bergh, N Fakas, N Grigoriadis, D Kalochristianakis, D Mitsikostas, A Orologas, A Tavernarakis, T Thomaidis, K Kovacs, K Matyas, P Piros, M Satori, K Anand, A Shifrin, K Banaszkiewicz, R Bonek, M Chahwan, M Czernichowska-Kotiuszko, L Darda-Ledzion, J Debrowska-Wójcik, M Dziki, E Krzystanek, M Kulka, P Lisewski, M Ratajczak, A Szczudlik, J Szczygiel, M Tomaszewska, J Wójcik, D Zielonka, M Chiru, S Deme, S Manescu, S M Nica, C Popescu, S Szatmari, A Fedyanin, N Malkova, D Popov, L Volkova, O Vorobeva, M Brozman, A Cimprichova, P Cuchran, L Gurcik, G Krastev, I Lisá, M Nyeky, J Poljaková, P Turcani, A Frost, J Heckmann, E Agüera, F Coret, A Escartin, V Fernandez, Jr Ara Callizo, G Martin, J E Martinez-Rodriguez, M Martinez Gines, D Munoz, J Olascoaga, J Prieto, C Ramo-Tello, S Belal, S Ben Ammou, M Frih-Ayed, R Gouider, C Mhiri, R Mrissa, A Cherkez, H Chmyr, L Chudovska, S Datskevych, L Dziak, A Galusha, M Khavunka, T Kobys, O Kozyolkin, Y Lekomtseva, T Litovchenko, O Moroz, G Moskovko, V Pashkovsky, Y Sanotskyi, S Shkrobot, T Braley, J Conway, B Hughes, A Katz, S Rizvi, R Singer

Affiliations

¹ From the Univ. Lille (P.V.), UMR Inserm U1172, CHU Lille, FHU Precise, France; Neurology Department (L.B.-R.), Hospital Arnau de Vilanova de Lleida, Spain; Mellen Center for Multiple Sclerosis (R.J.F.), Neurological Institute, Cleveland Clinic, OH; Experimental and Clinical Research Center and NeuroCure Clinical Research Center (F.P.), Max Delbrueck Center for Molecular Medicine and Charité Universitaetsmedizin Berlin, corporate member of Freie Universität Berlin, Humboldt-Universität zu Berlin, and Berlin Institute of Health, Germany; Neurology Department (L.R.-T.), Dr Josep Trueta University Hospital, Girona; Neurodegeneration and Neuroinflammation Research Group (L.R.-T.), IDIBGI, Salt; Medical Science Department (L.R.-T.), University of Girona, Spain; Neurology Department (M.S.), Jena University Hospital, Germany; AB Science (A.M., C.M., O.H.), Paris, France; Imagine Institute (O.H.), INSERM UMR 1163, Laboratory of Cellular and Molecular Mechanisms of Hematological Disorders and Therapeutic Implication, Hôpital Necker, Paris, France; and MA LEK AM Maciejowscy SC Centrum Terapii SM (M.M.), Katowice, Poland. patrick.vermersch@univ-lille.fr.
² From the Univ. Lille (P.V.), UMR Inserm U1172, CHU Lille, FHU Precise, France; Neurology Department (L.B.-R.), Hospital Arnau de Vilanova de Lleida, Spain; Mellen Center for Multiple Sclerosis (R.J.F.), Neurological Institute, Cleveland Clinic, OH; Experimental and Clinical Research Center and NeuroCure Clinical Research Center (F.P.), Max Delbrueck Center for Molecular Medicine and Charité Universitaetsmedizin Berlin, corporate member of Freie Universität Berlin, Humboldt-Universität zu Berlin, and Berlin Institute of Health, Germany; Neurology Department (L.R.-T.), Dr Josep Trueta University Hospital, Girona; Neurodegeneration and Neuroinflammation Research Group (L.R.-T.), IDIBGI, Salt; Medical Science Department (L.R.-T.), University of Girona, Spain; Neurology Department (M.S.), Jena University Hospital, Germany; AB Science (A.M., C.M., O.H.), Paris, France; Imagine Institute (O.H.), INSERM UMR 1163, Laboratory of Cellular and Molecular Mechanisms of Hematological Disorders and Therapeutic Implication, Hôpital Necker, Paris, France; and MA LEK AM Maciejowscy SC Centrum Terapii SM (M.M.), Katowice, Poland.

Abstract

Background and objectives: Masitinib is a selective tyrosine kinase inhibitor, targeting innate immune cells (mast cells and microglia) that are involved in the pathophysiology of progressive multiple sclerosis (MS). Study AB07002 assessed oral masitinib in patients with progressive MS who were progressing but not clinically active.

Methods: This randomized, double-blind, 2 parallel-group, placebo-controlled trial assessing 2 dose levels of masitinib vs equivalent placebo was conducted at 116 hospital clinics and specialized MS centers in 20 countries. Randomization (2:1) with minimization was performed centrally using an automated system. Patients, physicians, and outcome assessors remained masked to treatment group allocation. Patients with primary progressive MS (PPMS) or nonactive secondary progressive MS (nSPMS) without relapse for ≥2 years, aged 18-75 years, with baseline Expanded Disability Status Scale (EDSS) 2.0-6.0, and regardless of time from onset were treated for 96 weeks. The primary end point was overall EDSS change from baseline using repeated measures (generalized estimating equation, timeframe W12-W96, measured every 12 weeks), with positive values indicating increased clinical deterioration. Efficacy and safety were assessed in all randomly assigned and treated patients.

Results: A total of 611 patients were randomized; 301 in the masitinib 4.5 mg/kg/d parallel group and 310 in the uptitrated masitinib 6.0 mg/kg/d parallel group. Masitinib (4.5 mg/kg/d) (n = 199) showed significant benefit over placebo (n = 101) according to the primary end point, 0.001 vs 0.098, respectively, with a between-group difference of -0.097 (97% CI -0.192 to -0.002); p = 0.0256. Safety was consistent with masitinib's known profile (diarrhea, nausea, rash, and hematologic events), with no elevated risk of infection. Efficacy results from the independent uptitrated masitinib 6.0 mg/kg/d parallel group were inconclusive, and no new safety signal was observed.

Discussion: Masitinib (4.5 mg/kg/d) can benefit people with PPMS and nSPMS. A confirmatory phase 3 study will be initiated to substantiate these data.

Trial registration information: The first participant was randomized to study AB07002 on August 25, 2011. The trial was registered with the European Clinical Trials Database (#EudraCT 2010-021219-17) on July 1, 2011 (clinicaltrialsregister.eu/ctr-search/trial/2010-021219-17/ES) and with ClinicalTrials.gov (#NCT01433497) on September 14, 2011 (clinicaltrials.gov/ct2/show/NCT01433497).

Classification of evidence: This study provides Class II evidence that masitinib 4.5 mg/kg/d decreased progression of disability, measured by the EDSS, in adults with PPMS or patients with nSPMS (with no exacerbations in the last 2 years).

Publication types

Clinical Trial, Phase III
Randomized Controlled Trial
Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Adult
Benzamides / administration & dosage
Benzamides / adverse effects
Benzamides / pharmacology*
Disease Progression*
Double-Blind Method
Female
Humans
Male
Middle Aged
Multiple Sclerosis, Chronic Progressive / drug therapy*
Outcome Assessment, Health Care
Piperidines / administration & dosage
Piperidines / adverse effects
Piperidines / pharmacology*
Protein Kinase Inhibitors / administration & dosage
Protein Kinase Inhibitors / adverse effects
Protein Kinase Inhibitors / pharmacology*
Pyridines / administration & dosage
Pyridines / adverse effects
Pyridines / pharmacology*
Thiazoles / administration & dosage
Thiazoles / adverse effects
Thiazoles / pharmacology*
Young Adult

Substances

Benzamides
Piperidines
Protein Kinase Inhibitors
Pyridines
Thiazoles
masitinib

Associated data

ClinicalTrials.gov/NCT01433497
EudraCT/EudraCT 2010-021219-17