Mellen Center for MS Treatment and Research, Cleveland Clinic, Cleveland, OH, USA.
NeuroRx Research and Montreal Neurological Institute, Department of Neurology and Neurosurgery, McGill University, Montreal, QC, Canada.
Lancet Neurol. 2016 Apr;15(4):373-81. doi: 10.1016/S1474-4422(16)00018-1. Epub 2016 Feb 12.
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.
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.
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.
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.
Receptos, Inc.
以非选择性方式调节鞘氨醇 1-磷酸(S1P)受体可降低多发性硬化症患者的疾病活动度,但存在潜在的安全性问题。我们评估了口服选择性 S1P 受体调节剂奥扎尼莫德在复发性多发性硬化症患者中的安全性和疗效。
RADIANCE 是一项联合的 2/3 期试验。从欧洲和美国的 13 个国家的 55 个学术和私人多发性硬化症诊所招募了复发性多发性硬化症患者。合格的参与者年龄在 18-55 岁之间,扩展残疾状况量表(EDSS)评分为 0-5.0,且在筛选前 12 个月内有 1 次或多次复发,或过去 24 个月内有 1 次或多次复发,且在过去 12 个月内有 1 次或多次钆增强 MRI 病变。参与者按计算机生成的随机序列以 1:1:1 的比例随机分配至奥扎尼莫德(0.5mg 或 1mg)或匹配的安慰剂,每天一次,共 24 周,由独立的、不设盲的统计团队进行。试验参与者、研究现场人员、MRI 评估人员、指导委员会成员和研究统计学家均对治疗分配设盲。为减轻首剂心脏效应,奥扎尼莫德在 8 天内从 0.25mg 逐渐增加至 0.5mg 或 1mg。主要终点是治疗开始后 12-24 周由独立的 MRI 分析中心测量的总钆增强 MRI 病变累积数。分析采用意向治疗。在此,我们报告了 24 周 2 期试验的结果。该试验在 ClinicalTrials.gov 上注册,编号为 NCT01628393。正在进行为期 2 年的 3 期试验。
首位患者于 2012 年 10 月 18 日随机分组,最后一位随机分组患者的最后一次就诊时间为 2014 年 5 月 11 日。意向治疗和安全性人群包括 258 名参与者,88 名接受安慰剂,87 名接受奥扎尼莫德 0.5mg,83 名接受奥扎尼莫德 1mg;252(98%)名患者完成了指定的治疗。与安慰剂相比,奥扎尼莫德 0.5mg 组在治疗后 12-24 周时的平均累积钆增强病变数为 11.1(29.9),奥扎尼莫德 0.5mg 组为 1.5(3.7)(比值比 0.16,95%CI 0.08-0.30;p<0.0001),奥扎尼莫德 1mg 组为 1.5(3.4)(比值比 0.11,95%CI 0.06-0.21;p<0.0001)。在接受奥扎尼莫德 0.5mg 治疗的患者中,有 3 例与治疗无关的严重不良事件报告:视神经炎、躯体自主神经功能障碍和宫颈鳞状化生(HPV 相关)。未报告严重感染或心脏不良事件,也未发生黄斑水肿。奥扎尼莫德 0.5mg 和 1mg 组与安慰剂组相比,最常见的不良反应是鼻咽炎(11 例和 5 例比 12 例)、头痛(5 例和 3 例比 8 例)和尿路感染(6 例和 2 例比 2 例)。奥扎尼莫德治疗组在最初 6 小时内通过动态心电图监测的平均心率最大降低幅度小于 2 次/分钟(bpm),与基线相比,没有患者的最小每小时心率低于 45bpm。心电图和 24 小时动态心电图监测显示奥扎尼莫德没有增加房室传导阻滞或窦性暂停的发生率。
奥扎尼莫德显著降低了复发性多发性硬化症患者的 MRI 病变活动度,在 24 周的时间内具有良好的安全性。这些发现支持正在进行的 3 期试验。
Receptos,Inc.
