Ormrod D, McClellan K
Adis International Limited, Auckland, New Zealand.
Paediatr Drugs. 2001;3(4):293-319. doi: 10.2165/00128072-200103040-00006.
Topiramate is an antiepileptic drug (AED) which appears to have a broad range of antiseizure activity in humans. A previous overview focused primarily on results of trials of topiramate in adults with epilepsy, and this review highlights the use of topiramate in children. Clinical trials have shown that topiramate is effective when used adjunctively in children with refractory partial-onset seizures and generalised tonic-clonic seizures. The drug significantly reduced seizure frequency compared with placebo in children with partial-onset epilepsy after 16 weeks of double-blind adjunctive treatment (33.1 vs 10.5%); the frequency of secondarily generalised seizures was also markedly reduced. During a nonblind extension of this trial, the mean dosage was titrated from 4.8 to 9 mg/kg/day and further reductions in the frequency of seizures were observed (71% compared with prestudy levels). In 2 mixed adult/paediatric populations with primary generalised tonic-clonic seizures, topiramate (target dosage 5.2 to 9.3 mg/kg/day) reduced the seizure rate compared with those receiving placebo. This difference was significant in one trial (56.7 vs 9%) but not in another (57.1 vs 33.2%). A subanalysis of the paediatric patients found that the favourable effect of topiramate on seizure rates was not age-related. Topiramate (median average dosage 5.1 mg/kg/day) was also found to be useful as adjunctive therapy in the management of Lennox-Gastaut syndrome and significantly reduced the mean frequency of drop attacks by 14.8% compared with an increase of 5.1% with placebo. Further gains in seizure control were made in a nonblind extension of this trial where the mean topiramate dosage was 10 mg/kg/day. Nine of 11 patients in 1 pilot trial of children with otherwise intractable West syndrome, and 5 of 10 in another, achieved a > or =50% reduction in seizure rate with topiramate (target dosage up to 24 mg/kg/day). In an 18-month extension of the former trial (mean dosage 29 mg/kg/day) a > or =50% reduction in seizures was maintained in 7 of 11 children. Adverse events associated with adjunctive topiramate therapy in children were predominantly neuropsychiatric and generally mild to moderate in severity. Behavioural and cognitive problems do occur and are a limiting factor in some children. Also, weight loss can be problematical in some individuals. Withdrawal rates were low in the controlled trials (4.8%), but appear to be more frequent in noncomparative and post-marketing studies.
Well controlled studies have demonstrated that topiramate is an effective agent for the adjunctive therapy of partial and generalised tonic-clonic seizures in children. Treatment-limiting adverse events do occur, but these may be managed by slow titration. Although comparative studies with the other newer AEDs used in adjuntive therapy are required, topiramate is an important extension to the range of drugs that may be used to treat refractory epilepsy in children.
托吡酯是一种抗癫痫药物(AED),在人类中似乎具有广泛的抗癫痫发作活性。先前的综述主要关注托吡酯在成人癫痫试验中的结果,而本综述重点介绍托吡酯在儿童中的应用。临床试验表明,托吡酯在难治性部分性发作和全身性强直-阵挛性发作的儿童中作为辅助治疗有效。在双盲辅助治疗16周后,与安慰剂相比,托吡酯显著降低了部分性发作癫痫儿童的发作频率(33.1%对10.5%);继发性全身性发作的频率也显著降低。在该试验的非盲延长期,平均剂量从4.8毫克/千克/天滴定至9毫克/千克/天,观察到发作频率进一步降低(与研究前水平相比降低了71%)。在2个原发性全身性强直-阵挛性发作的成人/儿童混合人群中,与接受安慰剂的人群相比,托吡酯(目标剂量5.2至9.3毫克/千克/天)降低了发作率。在一项试验中这种差异具有显著性(56.7%对9%),但在另一项试验中并非如此(57.1%对33.2%)。对儿科患者的亚分析发现,托吡酯对发作率的有利影响与年龄无关。托吡酯(中位平均剂量5.1毫克/千克/天)在Lennox-Gastaut综合征的管理中作为辅助治疗也很有用,与安慰剂使跌倒发作频率增加5.1%相比,显著降低了跌倒发作的平均频率14.8%。在该试验的非盲延长期,托吡酯平均剂量为10毫克/千克/天,癫痫控制取得了进一步进展。在一项针对其他方面难治性West综合征儿童的试验中,11名患者中有9名,另一项试验中10名患者中有5名,使用托吡酯(目标剂量高达24毫克/千克/天)使发作率降低了≥50%。在前一项试验的18个月延长期(平均剂量29毫克/千克/天),11名儿童中有7名维持了发作降低≥50%。与儿童托吡酯辅助治疗相关的不良事件主要是神经精神性的,严重程度一般为轻度至中度。行为和认知问题确实会发生,并且在一些儿童中是一个限制因素。此外,体重减轻在一些个体中可能是个问题。在对照试验中撤药率较低(4.8%),但在非对照和上市后研究中似乎更频繁。
严格控制的研究表明,托吡酯是儿童部分性和全身性强直-阵挛性发作辅助治疗的有效药物。确实会发生限制治疗的不良事件,但这些可以通过缓慢滴定来处理。尽管需要与用于辅助治疗的其他新型抗癫痫药物进行比较研究,但托吡酯是可用于治疗儿童难治性癫痫的药物范围的重要扩展。
