儿童失神癫痫中抗癫痫药物疗效的药物遗传学
Pharmacogenetics of antiepileptic drug efficacy in childhood absence epilepsy.
作者信息
Glauser Tracy A, Holland Katherine, O'Brien Valerie P, Keddache Mehdi, Martin Lisa J, Clark Peggy O, Cnaan Avital, Dlugos Dennis, Hirtz Deborah G, Shinnar Shlomo, Grabowski Gregory
机构信息
Comprehensive Epilepsy Center, Division of Neurology, Cincinnati Children's Hospital Medical Center, Cincinnati, OH.
University of Cincinnati College of Medicine, Cincinnati, OH.
出版信息
Ann Neurol. 2017 Mar;81(3):444-453. doi: 10.1002/ana.24886.
OBJECTIVE
To determine whether common polymorphisms in CACNA1G, CACNA1H, CACNA1I, and ABCB1 are associated with differential short-term seizure outcome in childhood absence epilepsy (CAE).
METHODS
Four hundred forty-six CAE children in a randomized double-blind trial of ethosuximide, lamotrigine, and valproate had short-term seizure outcome determined. Associations between polymorphisms (minor allele frequency ≥ 15%) in 4 genes and seizure outcomes were assessed. In vitro electrophysiology on transfected CACNA1H channels determined impact of 1 variant on T-type calcium channel responsiveness to ethosuximide.
RESULTS
Eighty percent (357 of 446) of subjects had informative short-term seizure status (242 seizure free, 115 not seizure free). In ethosuximide subjects, 2 polymorphisms (CACNA1H rs61734410/P640L, CACNA1I rs3747178) appeared more commonly among not-seizure-free participants (p = 0.011, odds ratio [OR] = 2.63, 95% confidence limits [CL] = 1.25-5.56; p = 0.026, OR = 2.38, 95% CL = 1.11-5.00). In lamotrigine subjects, 1 ABCB1 missense polymorphism (rs2032582/S893A; p = 0.015, OR = 2.22, 95% CL = 1.16-4.17) was more common in not-seizure-free participants, and 2 CACNA1H polymorphisms (rs2753326, rs2753325) were more common in seizure-free participants (p = 0.038, OR = 0.52, 95% CL = 0.28-0.96). In valproate subjects, no common polymorphisms were associated with seizure status. In vitro electrophysiological studies showed no effect of the P640L polymorphism on channel physiology in the absence of ethosuximide. Ethosuximide's effect on rate of decay of Ca 3.2 was significantly less for P640L channel compared to wild-type channel.
INTERPRETATION
Four T-type calcium channel variants and 1 ABCB1 transporter variant were associated with differential drug response in CAE. The in vivo P640L variant's ethosuximide effect was confirmed by in vitro electrophysiological studies. This suggests that genetic variation plays a role in differential CAE drug response. Ann Neurol 2017;81:444-453.
目的
确定CACNA1G、CACNA1H、CACNA1I和ABCB1基因的常见多态性是否与儿童失神癫痫(CAE)短期癫痫发作结局差异相关。
方法
对446例参与乙琥胺、拉莫三嗪和丙戊酸盐随机双盲试验的CAE患儿进行短期癫痫发作结局判定。评估4个基因中的多态性(次要等位基因频率≥15%)与癫痫发作结局之间的关联。对转染的CACNA1H通道进行体外电生理学研究,确定1个变异对T型钙通道对乙琥胺反应性的影响。
结果
80%(446例中的357例)受试者具有可提供信息的短期癫痫发作状态(242例无癫痫发作,115例有癫痫发作)。在乙琥胺治疗组中,2种多态性(CACNA1H rs61734410/P640L、CACNA1I rs3747178)在有癫痫发作的参与者中更为常见(p = 0.011,优势比[OR]=2.63,95%置信区间[CL]=1.25 - 5.56;p = 0.026,OR = 2.38,95% CL = 1.11 - 5.00)。在拉莫三嗪治疗组中,1种ABCB1错义多态性(rs2032582/S893A;p = 0.015,OR = 2.22,95% CL = 1.16 - 4.17)在有癫痫发作的参与者中更为常见,而2种CACNA1H多态性(rs2753326、rs2753325)在无癫痫发作的参与者中更为常见(p = 0.038,OR = 0.52,95% CL = 0.28 - 0.�6)。在丙戊酸盐治疗组中,无常见多态性与癫痫发作状态相关。体外电生理学研究表明在无乙琥胺的情况下,P640L多态性对通道生理学无影响。与野生型通道相比,P640L通道中乙琥胺对Ca 3.2衰减速率的影响明显较小。
解读
4种T型钙通道变异和1种ABCB1转运体变异与CAE中的药物反应差异相关。体内P640L变异对乙琥胺的作用通过体外电生理学研究得到证实。这表明基因变异在CAE药物反应差异中起作用。《神经病学纪事》2017年;81:444 - 453。
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