1] Epilepsy Research Laboratory, Department of Neurological Surgery, University of California, San Francisco, Box 0520, 513 Parnassus Avenue San Francisco, California 94143, USA [2] Eli and Edythe Broad Center of Regeneration Medicine and Stem Cell Research, University of California, San Francisco, San Francisco, California 94143, USA.
Nat Commun. 2013;4:2410. doi: 10.1038/ncomms3410.
Dravet syndrome is a catastrophic pediatric epilepsy with severe intellectual disability, impaired social development and persistent drug-resistant seizures. One of its primary monogenic causes are mutations in Nav1.1 (SCN1A), a voltage-gated sodium channel. Here we characterize zebrafish Nav1.1 (scn1Lab) mutants originally identified in a chemical mutagenesis screen. Mutants exhibit spontaneous abnormal electrographic activity, hyperactivity and convulsive behaviours. Although scn1Lab expression is reduced, microarray analysis is remarkable for the small fraction of differentially expressed genes (~3%) and lack of compensatory expression changes in other scn subunits. Ketogenic diet, diazepam, valproate, potassium bromide and stiripentol attenuate mutant seizure activity; seven other antiepileptic drugs have no effect. A phenotype-based screen of 320 compounds identifies a US Food and Drug Administration-approved compound (clemizole) that inhibits convulsive behaviours and electrographic seizures. This approach represents a new direction in modelling pediatric epilepsy and could be used to identify novel therapeutics for any monogenic epilepsy disorder.
德拉维雷综合征是一种严重的儿童癫痫,伴有严重的智力残疾、社交发育障碍和持续的药物抵抗性癫痫发作。其主要的单基因病因之一是电压门控钠离子通道 Nav1.1(SCN1A)的突变。在这里,我们对最初在化学诱变筛选中鉴定出的斑马鱼 Nav1.1(scn1Lab)突变体进行了表征。突变体表现出自发性异常脑电图活动、过度活跃和惊厥行为。尽管 scn1Lab 的表达减少,但微阵列分析显示差异表达基因的比例很小(约 3%),并且其他 scn 亚基没有代偿性表达变化。生酮饮食、地西泮、丙戊酸钠、溴化钾和司替戊醇可减轻突变体的癫痫发作活动;其他七种抗癫痫药物则没有效果。基于表型的 320 种化合物筛选鉴定出一种美国食品和药物管理局批准的化合物(clemizole),可抑制惊厥行为和脑电图发作。这种方法代表了一种新的儿童癫痫模型方法,可用于鉴定任何单基因癫痫疾病的新型治疗药物。
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