Objective: To report safety and efficacy outcomes from up to 9 years of treatment with teriflunomide in an extension (NCT00803049) of the pivotal phase 3 Teriflunomide Multiple Sclerosis Oral (TEMSO) trial (NCT00134563).
Methods: A total of 742 patients entered the extension. Teriflunomide-treated patients continued the original dose; those previously
receiving placebo were randomized 1:1 to teriflunomide 14 mg or 7 mg.
Results: By June
2013, median (maximum) teriflunomide exposure exceeded 190 (325) weeks
per patient; 468 patients (63%) remained on
treatment. Teriflunomide was well-tolerated with
continued exposure. The most common adverse events (AEs) matched those
in
the core study. In extension year 1, first AEs
of transient liver enzyme increases or reversible hair thinning were
generally
attributable to patients switching from placebo
to teriflunomide. Approximately 11% of patients discontinued treatment
owing
to AEs. Twenty percent of patients experienced
serious AEs. There were 3 deaths unrelated to teriflunomide. Soon after
the
extension started, annualized relapse rates and
gadolinium-enhancing T1 lesion counts fell in patients switching from
placebo
to teriflunomide, remaining low thereafter.
Disability remained stable in all treatment groups (median Expanded
Disability
Status Scale score ≤2.5; probability of 12-week
disability progression ≤0.48).
Conclusions: In the
TEMSO extension, safety observations were consistent with the core
trial, with no new or unexpected AEs in patients
receiving teriflunomide for up to 9 years.
Disease activity decreased in patients switching from placebo and
remained low
in patients continuing on teriflunomide.
Classification of evidence:
This study provides Class III evidence that long-term treatment with
teriflunomide is well-tolerated and efficacy of teriflunomide
is maintained long-term.
Neurology 2016
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