NYU Comprehensive Epilepsy Center, New York, NY 10016, USA.
Neurology. 2010 Aug 10;75(6):519-25. doi: 10.1212/WNL.0b013e3181ec7f7f. Epub 2010 Jun 30.
To explore efficacy and safety/tolerability of adjunctive brivaracetam (BRV), a novel, high-affinity synaptic vesicle protein 2A ligand, which also inhibits neuronal voltage-dependent sodium channels, in patients with refractory partial-onset seizures (POS).
This was an exploratory, phase IIb, double-blind, randomized, parallel-group, placebo-controlled, dose-ranging study in patients 16-65 years with epilepsy experiencing > or =4 POS during 4-week baseline despite 1-2 concomitant antiepileptic drugs. Patients were randomized (1:1:1:1) to placebo, BRV 5 mg/day (BRV5), BRV 20 mg/day (BRV20), or BRV 50 mg/day (BRV50), administered BID without uptitration during a 7-week treatment period. Primary efficacy endpoint was POS frequency/week during the treatment period relative to placebo.
A total of 208 patients constituted the intention-to-treat population; 197 completed the study. Estimated percentage reductions over placebo in POS frequency/week were 9.8% (BRV5; p = 0.240), 14.9% (BRV20; p = 0.062), and 22.1% (BRV50; p = 0.004). Median percent reductions from baseline in POS frequency/week were 21.7% (placebo), 29.9% (BRV5; p = 0.086), 42.6% (BRV20; p = 0.014), and 53.1% (BRV50; p < 0.001); > or =50% responder rates were 16.7% (placebo), 32.0% (BRV5; p = 0.047), 44.2% (BRV20; p = 0.002), and 55.8% (BRV50; p < 0.001); seizure freedom rates (POS) during the 7-week treatment period were 1.9% (placebo), 8.0% (BRV5; p = 0.193), 7.7% (BRV20; p = 0.193), and 7.7% (BRV50; p = 0.201). BRV was well-tolerated. Most adverse events were mild to moderate and occurred with similar incidence in placebo and BRV groups, and discontinuations due to treatment-emergent adverse events were infrequent (placebo 3.7%; BRV 2.6%).
This interventional study provides preliminary Class I evidence that adjunctive BRV was efficacious and well-tolerated in patients aged 16-65 years with POS.
探讨新型高亲和力突触囊泡蛋白 2A 配体(BRV)联合用药的疗效和安全性/耐受性,BRV 还能抑制神经元电压依赖性钠通道,用于治疗耐药性部分发作性癫痫(POS)患者。
这是一项探索性、IIb 期、双盲、随机、平行分组、安慰剂对照、剂量范围研究,纳入了年龄在 16-65 岁、患有癫痫且在 4 周基线期内经历>或=4 次 POS 发作的患者,尽管使用了 1-2 种抗癫痫药物。患者随机(1:1:1:1)分为安慰剂组、BRV 5 mg/天(BRV5)组、BRV 20 mg/天(BRV20)组或 BRV 50 mg/天(BRV50)组,在 7 周的治疗期间,每日两次给药,不进行滴定。主要疗效终点是治疗期间 POS 发作频率/周与安慰剂相比的变化。
共有 208 名患者构成意向治疗人群;197 名患者完成了研究。与安慰剂相比,POS 发作频率/周的估计百分比降低分别为 9.8%(BRV5;p=0.240)、14.9%(BRV20;p=0.062)和 22.1%(BRV50;p=0.004)。POS 发作频率/周的中位数百分比降低分别为 21.7%(安慰剂)、29.9%(BRV5;p=0.086)、42.6%(BRV20;p=0.014)和 53.1%(BRV50;p<0.001);>或=50%的应答率分别为 16.7%(安慰剂)、32.0%(BRV5;p=0.047)、44.2%(BRV20;p=0.002)和 55.8%(BRV50;p<0.001);7 周治疗期间的无癫痫发作率(POS)分别为 1.9%(安慰剂)、8.0%(BRV5;p=0.193)、7.7%(BRV20;p=0.193)和 7.7%(BRV50;p=0.201)。BRV 耐受性良好。大多数不良事件为轻度至中度,在安慰剂和 BRV 组中发生的频率相似,因治疗相关不良事件而停药的情况很少见(安慰剂 3.7%;BRV 2.6%)。
这项干预性研究提供了初步的 I 类证据,表明辅助使用 BRV 对 16-65 岁的 POS 患者是有效且耐受良好的。
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