辅助性布瓦西坦治疗继发性全面强直阵挛发作的疗效、安全性及耐受性:三项III期研究的汇总结果
Efficacy, safety, and tolerability of adjunctive brivaracetam for secondarily generalized tonic-clonic seizures: Pooled results from three Phase III studies.
作者信息
Moseley Brian D, Sperling Michael R, Asadi-Pooya Ali A, Diaz Anyzeila, Elmouft Sami, Schiemann Jimmy, Whitesides John
机构信息
Department of Neurology and Rehabilitation Medicine, University of Cincinnati, Cincinnati, OH, USA.
Department of Neurology, Thomas Jefferson University, Philadelphia, PA, USA.
出版信息
Epilepsy Res. 2016 Nov;127:179-185. doi: 10.1016/j.eplepsyres.2016.09.003. Epub 2016 Sep 3.
PURPOSE
Secondarily generalized tonic-clonic seizures (SGTCS) are among the most devastating types of seizures, contributing to increased morbidity and mortality. Brivaracetam (BRV), a selective, high-affinity ligand for synaptic vesicle 2A (SV2A), has been shown to be useful for the adjunctive treatment of focal seizures. We sought to determine its specific efficacy in treating SGTCS.
METHODS
Data were pooled from three Phase III studies (NCT00490035; NCT00464269; NCT01261325) of adults with focal seizures taking 1-2 antiepileptic drugs (AEDs) who received placebo or BRV 50-200mg/day without titration over a 12-week treatment period. We report efficacy and safety/tolerability data for the BRV therapeutic dose range (50-200 mg/day) in patients with focal seizures including baseline SGTCS.
RESULTS
Patients (efficacy population, N=409) had been diagnosed with epilepsy for a mean±standard deviation duration of 22.2±13.1years. Baseline median SGTCS frequency was 3.0 per 28days. The majority (293, 71.6%) had failed ≥2 AEDs prior to study enrollment. The median percent reduction from baseline in SGTCS frequency/28days was: placebo, 33.3%; BRV 50mg/day, 66.6% (p<0.001); BRV 100mg/day, 61.2% (p=0.002); and BRV 200mg/day, 82.1% (p<0.001). The ≥50% responder rate for SGTCS was: placebo, 33.0%; BRV 50mg/day, 61.3% (p=0.003); BRV 100mg/day, 55.0% (p<0.001); and BRV 200mg/day, 64.0% (p<0.001). Freedom from SGTCS was achieved by: placebo, 14.8%; BRV 50mg/day, 22.6%; BRV 100mg/day, 31.0%; and BRV 200mg/day, 36.0% of patients. Time to first SGTCS during the treatment period was longer in patients receiving BRV than placebo (26days vs 8days, hazard ratio 0.55, p<0.001). In the SGTCS safety population (N=487), treatment-emergent adverse events (TEAEs) were reported by 60.6% of patients receiving placebo vs 65.0% of patients receiving BRV ≥50mg/day. Serious TEAEs were reported by 3.1% placebo vs 3.9% BRV ≥50mg/day. Discontinuations due to TEAEs were 3.9% placebo vs 6.3% BRV ≥50mg/day.
CONCLUSIONS
In patients with drug-resistant focal seizures, adjunctive BRV is effective in reducing the frequency of SGTCS. Almost one-third (30.4%) of patients were rendered completely free of SGTCS during the 12-week treatment period when taking BRV ≥50mg/day. BRV was well tolerated, with a TEAE profile consistent with that of the overall study population.
目的
继发性全面强直阵挛发作(SGTCS)是最具破坏性的癫痫发作类型之一,会导致发病率和死亡率上升。布瓦西坦(BRV)是一种针对突触囊泡2A(SV2A)的选择性、高亲和力配体,已被证明可用于局灶性癫痫发作的辅助治疗。我们试图确定其治疗SGTCS的具体疗效。
方法
数据来自三项III期研究(NCT00490035;NCT00464269;NCT01261325),这些研究针对服用1 - 2种抗癫痫药物(AEDs)的局灶性癫痫发作成年患者,他们在12周的治疗期内接受了安慰剂或每天50 - 200mg的BRV,且未进行滴定。我们报告了BRV治疗剂量范围(50 - 200mg/天)在包括基线SGTCS的局灶性癫痫发作患者中的疗效以及安全性/耐受性数据。
结果
患者(疗效人群,N = 409)被诊断为癫痫的平均±标准差病程为22.2±13.1年。基线时SGTCS的中位数频率为每28天3.0次。大多数(293例,71.6%)患者在研究入组前使用≥2种AEDs治疗失败。SGTCS频率/每28天较基线降低的中位数百分比为:安慰剂组33.3%;BRV 50mg/天组66.6%(p < 0.001);BRV 100mg/天组61.2%(p = 0.002);BRV 200mg/天组82.1%(p < 0.001)。SGTCS的≥50%缓解率为:安慰剂组33.0%;BRV 50mg/天组61.3%(p = 0.003);BRV 100mg/天组55.0%(p < 0.001);BRV 200mg/天组64.0%(p < 0.001)。达到无SGTCS状态的比例为:安慰剂组14.8%;BRV 50mg/天组22.6%;BRV 100mg/天组31.0%;BRV 200mg/天组36.0%。接受BRV治疗的患者在治疗期间首次发生SGTCS的时间比接受安慰剂的患者更长(26天对8天,风险比0.55,p < 0.001)。在SGTCS安全性人群(N = 487)中,接受安慰剂的患者有60.6%报告了治疗期间出现的不良事件(TEAE),而接受≥50mg/天BRV的患者为65.0%。报告严重TEAE的比例在安慰剂组为3.1%,在BRV≥50mg/天组为3.9%。因TEAE停药的比例在安慰剂组为3.9%,在BRV≥50mg/天组为6.3%。
结论
在耐药性局灶性癫痫发作患者中,辅助使用BRV可有效降低SGTCS的频率。在服用≥50mg/天BRV的12周治疗期间,近三分之一(30.4%)的患者完全没有发生SGTCS。BRV耐受性良好,其TEAE情况与整个研究人群一致。
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