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抗惊厥药物的作用机制。

Anticonvulsant drug mechanisms of action.

作者信息

Macdonald R L, McLean M J, Skerritt J H

出版信息

Fed Proc. 1985 Jul;44(10):2634-9.

PMID:2408925
Abstract

The effects of clinically used anticonvulsant drugs on high-frequency sustained repetitive firing (SRF) of action potentials and on postsynaptic responses to iontophoretically applied gamma-aminobutyric acid (GABA) have been compared to establish a classification of anticonvulsant drugs based on cellular mechanisms of action. By using concentrations in the range of therapeutic cerebrospinal fluid values in humans, drugs have been separated into three categories: Phenytoin, carbamazepine, and valproic acid limited SRF, but did not alter GABA responses. Phenobarbital, clonazepam, and diazepam augmented GABA responses and limited SRF only at concentrations above the therapeutic range in ambulatory patients but that are achieved in the acute treatment of status epilepticus. Ethosuximide failed to affect SRF or GABA responses even at supratherapeutic concentrations. Ability of an anticonvulsant to limit SRF correlated well with efficacy against generalized tonic-clonic seizures clinically and against maximal electroshock seizures in experimental animals. Augmentation of GABA responses and lack of limitation of SRF correlated with efficacy against generalized absence seizures in humans and against pentylenetetrazol-induced seizures in animals. However, ethosuximide must act against generalized absence seizures and against pentylenetetrazol-induced seizures by a third, as yet unknown, mechanism. Other actions occurring at supratherapeutic concentrations correlated with clinical toxicity.

摘要

已比较了临床使用的抗惊厥药物对动作电位高频持续重复发放(SRF)以及对离子电渗法施加γ-氨基丁酸(GABA)后突触后反应的影响,以根据细胞作用机制对抗惊厥药物进行分类。通过使用人体治疗性脑脊液值范围内的浓度,药物被分为三类:苯妥英、卡马西平和丙戊酸限制SRF,但不改变GABA反应。苯巴比妥、氯硝西泮和地西泮增强GABA反应,且仅在高于门诊患者治疗范围但在癫痫持续状态急性治疗中可达到的浓度下限制SRF。乙琥胺即使在超治疗浓度下也未能影响SRF或GABA反应。抗惊厥药限制SRF的能力与临床上对全身性强直阵挛性发作以及实验动物最大电休克发作的疗效密切相关。GABA反应增强和SRF无限制与人类对全身性失神发作以及动物对戊四氮诱导发作的疗效相关。然而,乙琥胺对抗全身性失神发作和戊四氮诱导发作必须通过第三种尚未知晓的机制起作用。超治疗浓度下出现的其他作用与临床毒性相关。

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