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癫痫持续状态的发病机制、药理学特性及其新型抗癫痫药物治疗

Mechanistic and pharmacologic aspects of status epilepticus and its treatment with new antiepileptic drugs.

作者信息

Wasterlain Claude G, Chen James W Y

机构信息

Epilepsy Research Laboratories, Department of Neurology, David Gefen School of Medicine at UCLA, Los Angeles, California, USA.

出版信息

Epilepsia. 2008 Dec;49 Suppl 9:63-73. doi: 10.1111/j.1528-1167.2008.01928.x.

Abstract

We review recent advances in our understanding and treatment of status epilepticus (SE). Repeated seizures cause an internalization of gamma-aminobutyric acid (GABA)(A) receptors, together with a movement of N-methyl-d-aspartate (NMDA) receptors to the synapse. As a result, the response of experimental SE to treatment with GABAergic drugs (but not with NMDA antagonists) fades with increasing seizure duration. Prehospital treatment, which acts before these changes are established, is finding increased acceptance, and solid evidence of its efficacy is available, particularly in children. Rational polypharmacy aims at multiple receptors or ion channels to increase inhibition and simultaneously reduce excitation. Combining GABA(A) agonists with NMDA antagonists and with agents acting at other sites is successful in treating experimental SE, and in reducing SE-induced brain damage and epileptogenesis. The relevance of these experimental data to clinical SE is actively debated. Valproate and levetiracetam have recently become available for intravenous use, and the use of ketamine and of other agents (topiramate, felbamate, etc.) have seen renewed interest. A rapidly increasing but largely anecdotal body of literature reports success in seizure control at the price of relatively few complications with the clinical use of those agents in refractory SE.

摘要

我们回顾了目前在癫痫持续状态(SE)的认识和治疗方面取得的进展。反复癫痫发作会导致γ-氨基丁酸(GABA)(A)受体内化,同时N-甲基-D-天冬氨酸(NMDA)受体向突触移动。因此,随着癫痫发作持续时间的增加,实验性SE对GABA能药物(而非NMDA拮抗剂)治疗的反应逐渐减弱。在这些变化发生之前进行的院前治疗越来越被接受,并且有确凿的疗效证据,尤其是在儿童中。合理的联合用药旨在作用于多个受体或离子通道,以增强抑制作用并同时减少兴奋作用。将GABA(A)激动剂与NMDA拮抗剂以及作用于其他位点的药物联合使用,在治疗实验性SE以及减少SE诱导的脑损伤和癫痫发生方面取得了成功。这些实验数据与临床SE的相关性正受到积极讨论。丙戊酸盐和左乙拉西坦最近已可用于静脉注射,氯胺酮和其他药物(托吡酯、非氨酯等)的使用也重新引起了人们的兴趣。越来越多但大多为轶事性的文献报道,在难治性SE的临床使用中,这些药物以相对较少的并发症为代价成功控制了癫痫发作。

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