Background
Modulation of sphingosine
1-phosphate (S1P) receptors in a non-selective manner decreases disease
activity in patients with multiple sclerosis but has potential safety
concerns. We assessed the safety and efficacy of the oral selective S1P
receptor modulator ozanimod in patients with relapsing multiple
sclerosis.
Methods
RADIANCE is a
combined phase 2/3 trial. Patients with relapsing multiple sclerosis
were recruited from 55 academic and private multiple sclerosis clinics
in 13 countries across Europe and the USA. Eligible participants were
aged 18–55 years, had an Expanded Disability Status Scale (EDSS) score
of 0–5·0, and had either one or more relapses in the previous 12 months,
or one or more relapses in the past 24 months and one or more
gadolinium-enhancing lesions on MRI in the previous 12 months before
screening. Participants were assigned by a computer-generated
randomisation sequence in a 1:1:1 ratio to ozanimod (0·5 mg or 1 mg) or
matching placebo once daily for 24 weeks by an independent, unmasked,
statistical team. Trial participants, study site personnel, MRI
assessors, steering committee members, and the study statistician were
masked to treatment assignment. To attenuate first-dose cardiac effects,
ozanimod was up-titrated from 0·25 mg to 0·5 mg or 1 mg over 8 days.
The primary endpoint was the cumulative number of total
gadolinium-enhancing MRI lesions measured by an independent MRI analysis
centre at weeks 12–24 after treatment initiation. Analysis was by
intention to treat. Here, we report results from the 24-week phase 2
trial. This trial is registered with ClinicalTrials.gov, number NCT01628393. The 2-year phase 3 trial is ongoing.
Findings
The
first patient was randomised on Oct 18, 2012, and the final visit of
the last randomised patient was on May 11, 2014. The intention-to-treat
and safety population consisted of 258 participants, 88 were assigned
placebo, 87 ozanimod 0·5 mg, and 83 ozanimod 1 mg; 252 (98%) patients
completed the assigned treatment. The mean cumulative number of
gadolinium-enhancing lesions at weeks 12–24 was 11·1 (SD 29·9) with
placebo compared with 1·5 (3·7) with ozanimod 0·5 mg (odds ratio 0·16,
95% CI 0·08–0·30; p<0·0001) and 1·5 (3·4) with ozanimod 1 mg (odds
ratio 0·11, 95% CI 0·06–0·21; p<0·0001). Three serious adverse events
unrelated to treatment were reported in patients assigned ozanimod 0·5
mg: optic neuritis, somatoform autonomic dysfunction, and cervical
squamous metaplasia (HPV-related). No serious infectious or cardiac
adverse events were reported, and no cases of macular oedema arose. The
most common adverse events in the ozanimod 0·5 mg and 1 mg groups
compared with placebo were nasopharyngitis (11 and five vs 12), headache (five and three vs eight), and urinary-tract infections (six and two vs
two). The maximum reduction in mean heart rate by Holter monitoring
during the first 6 h in ozanimod-treated participants was less than 2
beats per min (bpm) compared with baseline, with no patient having a
minimum hourly heart rate less than 45 bpm. Electrocardiograms and 24-h
Holter monitoring showed no increased incidence of atrioventricular
block or sinus pause with ozanimod.
Interpretation
Ozanimod
significantly reduced MRI lesion activity in participants with
relapsing multiple sclerosis, with a favourable safety profile over a
period of 24 weeks. These findings warrant phase 3 trials, which are
ongoing.
Lancet Neurology 2016
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