| Literature DB >> 25878002 |
Mark S Freedman1, Giancarlo Comi2, Nicola De Stefano3, Frederik Barkhof4, Chris H Polman4, Bernard M J Uitdehaag4, Lorenz Lehr5, Bettina Stubinski5, Ludwig Kappos6.
Abstract
The first clinical presentation of multiple sclerosis (MS) is usually a single episode of typical symptoms and signs and is designated a "first clinical demyelinating event" (FCDE) or a "clinically isolated syndrome". Patients with an FCDE who show 'silent' magnetic resonance imaging lesions are at high risk of further clinical events and therefore of meeting the criteria for the diagnosis of clinically definite MS (CDMS). Here we review five Phase III trials, in which treatment with the following disease-modifying drugs (DMDs) was initiated at this early stage: interferon beta (ETOMS, CHAMPS, BENEFIT, and REFLEX) and glatiramer acetate (PreCISe). Differences in the design of the trials and their patient inclusion criteria limit comparisons. However, the proportion of placebo-treated patients who developed CDMS within 2 years was 38-45% across studies, and this rate was significantly reduced by DMD treatment. Conversion to McDonald MS was reported by only two of the trials: BENEFIT (2001 criteria) and REFLEX (2005 criteria). Around 85% of placebo-treated patients developed McDonald MS by 2 years in each, and again a beneficial effect of DMD treatment was seen. Overall, these studies support early use of DMDs to treat patients with an FCDE who are at high risk of conversion to CDMS.Entities:
Keywords: Clinically isolated syndrome; Disease-modifying drug; First clinical demyelinating event; Glatiramer acetate; Interferon beta; Multiple sclerosis
Year: 2013 PMID: 25878002 DOI: 10.1016/j.msard.2013.07.001
Source DB: PubMed Journal: Mult Scler Relat Disord ISSN: 2211-0348 Impact factor: 4.339