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氯咪唑和5-羟色胺信号调节剂可抑制德雷维特综合征中的癫痫发作。

Clemizole and modulators of serotonin signalling suppress seizures in Dravet syndrome.

作者信息

Griffin Aliesha, Hamling Kyla R, Knupp Kelly, Hong SoonGweon, Lee Luke P, Baraban Scott C

机构信息

Epilepsy Research Laboratory and Weill Institute for Neurosciences, Department of Neurological Surgery, University of California, San Francisco, San Francisco, CA, USA.

Department of Pediatrics, University of Colorado Denver, Denver, CO, USA.

出版信息

Brain. 2017 Mar 1;140(3):669-683. doi: 10.1093/brain/aww342.

Abstract

Dravet syndrome is a catastrophic childhood epilepsy with early-onset seizures, delayed language and motor development, sleep disturbances, anxiety-like behaviour, severe cognitive deficit and an increased risk of fatality. It is primarily caused by de novo mutations of the SCN1A gene encoding a neuronal voltage-activated sodium channel. Zebrafish with a mutation in the SCN1A homologue recapitulate spontaneous seizure activity and mimic the convulsive behavioural movements observed in Dravet syndrome. Here, we show that phenotypic screening of drug libraries in zebrafish scn1 mutants rapidly and successfully identifies new therapeutics. We demonstrate that clemizole binds to serotonin receptors and its antiepileptic activity can be mimicked by drugs acting on serotonin signalling pathways e.g. trazodone and lorcaserin. Coincident with these zebrafish findings, we treated five medically intractable Dravet syndrome patients with a clinically-approved serotonin receptor agonist (lorcaserin, Belviq®) and observed some promising results in terms of reductions in seizure frequency and/or severity. Our findings demonstrate a rapid path from preclinical discovery in zebrafish, through target identification, to potential clinical treatments for Dravet syndrome.

摘要

德雷维特综合征是一种严重的儿童癫痫,伴有早发性癫痫发作、语言和运动发育迟缓、睡眠障碍、焦虑样行为、严重认知缺陷以及死亡风险增加。它主要由编码神经元电压门控钠通道的SCN1A基因的新生突变引起。SCN1A同源物发生突变的斑马鱼重现了自发性癫痫活动,并模拟了德雷维特综合征中观察到的惊厥行为动作。在此,我们表明在斑马鱼scn1突变体中对药物文库进行表型筛选能够快速且成功地鉴定出新的治疗方法。我们证明氯苯咪唑与血清素受体结合,其抗癫痫活性可被作用于血清素信号通路的药物(如曲唑酮和洛卡塞林)模拟。与这些斑马鱼研究结果一致,我们用一种临床批准的血清素受体激动剂(洛卡塞林,Belviq®)治疗了五名药物难治性德雷维特综合征患者,并在癫痫发作频率和/或严重程度降低方面观察到了一些有前景的结果。我们的研究结果展示了一条从斑马鱼的临床前发现,经过靶点鉴定,到德雷维特综合征潜在临床治疗的快速路径。

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