Abstract
IntroductionSince current treatment options for patients suffering from active rheumatoid arthritis (RA) remain inadequate, especially for those unresponsive to disease-modifying antirheumatic drugs (DMARDs), new and improved medication is needed. This study evaluates the safety and efficacy of masitinib (AB1010), a potent and selective protein tyrosine kinase inhibitor of c-KIT, in the monotherapy treatment of DMARD-refractory RA.MethodsThis was a multicentre, uncontrolled, open-label, randomised, dose-ranging, phase 2a trial. Masitinib was administered orally to 43 patients who had inadequate response to DMARDs, at initial randomised dosing levels of 3 and 6 mg/kg per day over a 12-week period. Dose adjustment was permitted based upon tolerability and response criteria. Efficacy was assessed via American College of Rheumatology 20%/50%/70% improvement criteria (ACR20/50/70) responses, disease activity score using 28 joint counts (DAS28), index of improvement in RA (ACRn) and C-reactive protein (CRP) improvement, relative to baseline at week 12.ResultsImprovement was observed in all efficacy endpoints, including ACR20/50/70 scores of 54%, 26% and 8%, respectively, and a reduction in CRP level by greater than 50% for approximately half the population. This improvement was sustainable throughout an extension phase (> 84 weeks) and was also independent of initial DMARD resistance (anti-tumour necrosis factor-alpha and/or methotrexate). A relatively high patient withdrawal rate (37%) required the use of last observation carried forward (LOCF) data imputation. Incidence of adverse events was high (95%), although the majority were of mild or moderate severity with a considerable decline in frequency observed after 12 weeks of treatment. Two nonfatal serious adverse events were reported. Dose-response analyses tentatively indicate that an initial dosing level of 6.0 mg/kg per day administered orally in two daily intakes is the most appropriate, based upon potency and tolerability trends.ConclusionsTreatment with masitinib improved DMARD-refractory active RA. Following an initial high incidence of mostly mild to moderate side effects during the first 12 weeks of treatment, masitinib appears to be generally well tolerated. This, together with evidence of a sustainable efficacy response, suggests that masitinib is suitable for long-term treatment regimens. Since this was the first study of masitinib in a nononcologic pathology, the relatively high patient withdrawal rate observed can be partly attributed to a highly cautious response to adverse events. There is sufficient compelling evidence to warrant further placebo-controlled investigation.Trial registrationClinicalTrials.gov NCT00831922.
Highlights
Since current treatment options for patients suffering from active rheumatoid arthritis (RA) remain inadequate, especially for those unresponsive to diseasemodifying antirheumatic drugs (DMARDs), new and improved medication is needed
Improvement was observed in all efficacy endpoints, including ACR20/50/70 scores of 54%, 26% and 8%, respectively, and a reduction in C-reactive protein (CRP) level by greater than 50% for approximately half the population
This, ABL: Abelson kinase; ACR: American College of Rheumatology; ACR20/50/70/90: American College of Rheumatology 20%/50%/70%/90% improvement criteria; ACRn: index of improvement in rheumatoid arthritis; adverse events (AEs): adverse event; anti-TNFα: anti-tumour necrosis factor-alpha; CRP: Creactive protein; DAS28: disease activity score using 28 joint counts; DMARD: disease-modifying antirheumatic drug; IC50: half inhibitory concentration; IL1: interleukin-1; IL1 receptor antagonist (IL1-Ra): interleukin-1 receptor antagonist; ITT: intention-to-treat; LOCF: last observation carried forward; mast cells (MCs): mast cell; MTX: methotrexate; NSAID: nonsteroidal anti-inflammatory drug; OC: observed case; PDGFR: platelet-derived growth factor receptor; PP: per protocol; RA: rheumatoid arthritis; serious adverse events (SAEs): serious adverse event; Stem cell factor (SCF): stem cell factor; TK: tyrosine kinase
Summary
Since current treatment options for patients suffering from active rheumatoid arthritis (RA) remain inadequate, especially for those unresponsive to diseasemodifying antirheumatic drugs (DMARDs), new and improved medication is needed. A problem more general to DMARDs is that of drug resistance, which represents a major obstacle to the effective long-term management of RA [3] Both MTX [4] and anti-tumour necrosis factor-alpha (antiTNFα) [5] may become inefficient for controlling disease activity in severe RA. Beyond the already developed biological strategies, there exists an imperative need to identify alternative RA treatments that demonstrate high efficacy over time in monotherapy, exploit novel therapeutic targets for more effective combination therapies, minimise toxicity and are affordable. One such approach involves blocking intracellular proinflammatory messages, which is currently represented by the strategy of selective protein tyrosine kinase (TK) inhibition
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