Abstract

A critical issue in the management of relapsing MS (RMS) is the discontinuation of disease-modifying treatments (DMT) due to lack of efficacy, intolerability or impending risks. With new therapeutic agents introduced into the treatment of RMS, immediate- and long-term consequences of sequential drug use, as well as the effect of the sequence in which the drugs are given, are unclear but may affect efficacy, adverse events, and long-term immunocompetence. In the absence of clinical studies specifically addressing these concerns, observations from clinical practice are of particular value in guiding current management algorithms. Prompted by a study published by Ferraro et al. in this journal, we set out to provide an overview of the published real-world evidence on the effectiveness and safety of switching from fingolimod to another DMT in patients with active RMS. Seventeen publications reporting relevant information were identified. The literature suggests that immune cell depletion induced by alemtuzumab or ocrelizumab is associated with an increased risk of relapse and worsening disability in patients switching from fingolimod compared to patients switching from other therapeutic agents. However, the evidence reported for natalizumab and cladribine is inconclusive. While shortening of the washout period may limit early disease reactivation after fingolimod discontinuation, there is no strong evidence that the duration of the washout period or the absolute lymphocyte count at baseline are predictors of attenuated long-term efficacy. Further real-world studies are required to better understand outcomes among patients who are under-represented in controlled trials.

Highlights

  • The expansion of the treatment landscape in active relapsing multiple sclerosis (RMS) has led to increased complexity of treatment choices

  • Since prospective, randomized, controlled clinical trials are not available, this review summarized current real-world evidence regarding the best treatment switch strategy following fingolimod

  • Evidence for natalizumab is lacking and, as it carries the risk of progressive multifocal leukoencephalopathy (PML) development, it may not be a longer-term alternative

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Summary

Introduction

The expansion of the treatment landscape in active relapsing multiple sclerosis (RMS) has led to increased complexity of treatment choices. While several studies have examined this treatment strategy [2, 3]—the progression from first- to second-line therapy—evidence regarding a ‘lateral switch’ to a drug with comparable efficacy but different mode of action, following previous active treatment, remains scarce. This is mainly due to phase III clinical trials supporting the approval of these disease-modifying therapies (DMT) not usually including patients on prior active treatment. As guidelines do not make recommendation on this matter and clear data regarding treatment sequencing are missing, we consider it of utmost importance to give a compact overview of current data to help physicians in their daily routine when advising patients on fingolimod regarding a necessary ‘lateral switch’

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