Abstract
Secondary progressive multiple sclerosis, for which no satisfactory treatment presently exists, accounts for most of the disability in patients with multiple sclerosis. Simvastatin, which is widely used for treatment of vascular disease, with its excellent safety profile, has immunomodulatory and neuroprotective properties that could make it an appealing candidate drug for patients with secondary progressive multiple sclerosis. We undertook a double-blind, controlled trial between Jan 28, 2008, and Nov 4, 2011, at three neuroscience centres in the UK. Patients aged 18-65 years with secondary progressive multiple sclerosis were randomly assigned (1:1), by a centralised web-based service with a block size of eight, to receive either 80 mg of simvastatin or placebo. Patients, treating physicians, and outcome assessors were masked to treatment allocation. The primary outcome was the annualised rate of whole-brain atrophy measured from serial volumetric MRI. Analyses were by intention to treat and per protocol. This trial is registered with ClinicalTrials.gov, number NCT00647348. 140 participants were randomly assigned to receive either simvastatin (n=70) or placebo (n=70). The mean annualised atrophy rate was significantly lower in patients in the simvastatin group (0·288% per year [SD 0·521]) than in those in the placebo group (0·584% per year [0·498]). The adjusted difference in atrophy rate between groups was -0·254% per year (95% CI -0·422 to -0·087; p=0·003); a 43% reduction in annualised rate. Simvastatin was well tolerated, with no differences between the placebo and simvastatin groups in proportions of participants who had serious adverse events (14 [20%] vs nine [13%]). High-dose simvastatin reduced the annualised rate of whole-brain atrophy compared with placebo, and was well tolerated and safe. These results support the advancement of this treatment to phase 3 testing. The Moulton Foundation [charity number 1109891], Berkeley Foundation [268369], the Multiple Sclerosis Trials Collaboration [1113598], the Rosetrees Trust [298582] and a personal contribution from A Pidgley, UK National Institute of Health Research (NIHR) University College London Hospitals/UCL Biomedical Research Centres funding scheme.
Highlights
Multiple sclerosis is a major cause of disability, in young adults in temperate climates
Cholesterol was significantly reduced from mean 5·5 (SD 1·1) mmol/L at baseline to 4·1 (0·9) mmol/L at 24 months in the simvastatin group (p
At 24 months we recorded a statistically significant difference in favour of simvastatin versus placebo for Expanded Disability Severity Scale (EDSS) and total multiple sclerosis impact scale-29 (MSIS-29) (−4·78; 95% CI −9·39 to −0·02; p
Summary
Multiple sclerosis is a major cause of disability, in young adults in temperate climates. Despite much success with drugs that substantially reduce relapse frequency during the initial inflammatory, relapsingremitting phase, more than half of patients eventually develop non-relapsing, secondary progressive multiple sclerosis one to two decades after the onset of relapsingremitting multiple sclerosis. This relentless accumulation of neurological deficit and increasing brain atrophy is thought to be driven by neuroaxonal loss.[1] several symptomatic treatments are available, progression in secondary progressive multiple sclerosis is presently intractable. Direct neuroprotection strategies (eg, lamotrigine,[6] tetrahydrocannabinol7) have failed.[8] The crucial and as yet unmet challenge is to find effective and well-tolerated treatments for secondary progressive multiple sclerosis
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