Ramsay R Eugene, Perucca Emilio, Robbins Jefferey, Barrett Jeannette A, Spiegel Katharyn
Department of Neurology, University of Miami School of Medicine, Miami Veterans Affairs Medical Center, Miami, Florida, USA.
Epilepsia. 2009 Aug;50(8):1891-8. doi: 10.1111/j.1528-1167.2009.02148.x. Epub 2009 Jun 1.
To determine the time at which pregabalin demonstrates seizure-suppressing activity when given as adjunctive treatment to patients with refractory partial seizures.
Data from four similar 12-week, randomized, double-blind, placebo-controlled, parallel-group trials in patients with refractory partial seizures were pooled to provide an adequate sample to compare the proportion of patients free of seizures on each study day between pregabalin (combined 150-600 mg/day groups) and placebo (combined groups). A generalized estimating equation (GEE) statistical model was used to perform pairwise comparisons on each study day. In several pregabalin dosage groups the dosage was escalated during days 1-7, whereas in others pregabalin was initiated at a fixed dosage without escalation.
The proportion of patients free of seizures on any treatment day was greater in the combined pregabalin groups compared with baseline. Differences were not observed between the placebo group and baseline. A significantly greater proportion of patients were free of seizures in the combined pregabalin 150-600 mg/day and the pregabalin 600 mg/day fixed-dosage groups compared with the placebo groups from treatment day 2 onward (p < 0.05). From day 8 (coinciding with completion of the 1-week dosage-escalation period in two studies) onward, the proportion of patients free of seizures per day in the pregabalin groups remained relatively constant.
This exploratory analysis of a refractory population using a rigorous endpoint demonstrates that pregabalin rapidly reduced the frequency of partial seizures. At the dosing schemes most commonly used in placebo-controlled trials, significant seizure-suppressing activity was observed after only 2 days of treatment.
确定加巴喷丁作为难治性部分性癫痫患者辅助治疗药物时,出现癫痫抑制活性的时间。
汇总四项针对难治性部分性癫痫患者的相似的为期12周的随机、双盲、安慰剂对照平行组试验的数据,以提供足够样本,比较加巴喷丁(150 - 600 mg/天联合组)和安慰剂(联合组)在每个研究日无癫痫发作患者的比例。使用广义估计方程(GEE)统计模型在每个研究日进行两两比较。在几个加巴喷丁剂量组中,剂量在第1 - 7天逐步增加,而在其他组中,加巴喷丁以固定剂量起始且无剂量增加。
与基线相比,加巴喷丁联合组在任何治疗日无癫痫发作的患者比例更高。安慰剂组与基线之间未观察到差异。从治疗第2天起,加巴喷丁150 - 600 mg/天联合组和加巴喷丁600 mg/天固定剂量组中无癫痫发作的患者比例显著高于安慰剂组(p < 0.05)。从第8天(与两项研究中1周剂量递增期结束一致)起,加巴喷丁组中每日无癫痫发作的患者比例保持相对稳定。
使用严格终点对难治性人群进行的这项探索性分析表明,加巴喷丁能迅速降低部分性癫痫发作的频率。在安慰剂对照试验中最常用的给药方案下,仅治疗2天后就观察到了显著的癫痫抑制活性。