Mutation in SNAP25 as a novel genetic cause of epilepsy and intellectual disability.

Rare diseases (Austin, Tex.) Pub Date : 2013-09-05 eCollection Date: 2013-01-01 DOI:10.4161/rdis.26314

Luis Rohena, Julie Neidich, Megan Truitt Cho, Kelly Df Gonzalez, Sha Tang, Orrin Devinsky, Wendy K Chung

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引用次数: 60

Abstract

Whole exome sequencing using a parent-child trio design to identify de novo mutations provides an efficient method to identify novel genes for rare diseases with low reproductive fitness that are difficult to study by more classical genetic methods of linkage analysis. We describe a 15 y old female with severe static encephalopathy, intellectual disability, and generalized epilepsy. After extensive metabolic and genetic testing, whole exome sequencing identified a novel de novo variant in Synaptosomal-associated protein-25 (SNAP25), c.142G > T p.Phe48Val alteration. This variant is predicted to be damaging by all prediction algorithms. SNAP25 is part of the soluble N-ethylmaleimide-sensitive factor attachment protein receptor (SNARE) protein complex which is involved in exocytotic release of neurotransmitters. Genetic alterations in Snap25 in animal models can cause anxiety-related behavior, ataxia and seizures. We suggest that SNAP25 mutations in humans are a novel genetic cause of intellectual disability and epilepsy.

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SNAP25突变作为癫痫和智力残疾的新遗传原因。

采用亲子三重奏设计的全外显子组测序鉴定新生突变，为鉴定具有低生殖适应度的罕见疾病的新基因提供了一种有效的方法，这种方法难以通过更经典的连锁分析遗传方法进行研究。我们描述了一名15岁的女性，患有严重的静态脑病，智力残疾和全身性癫痫。经过广泛的代谢和基因检测，全外显子组测序鉴定出突触体相关蛋白25 (SNAP25)的一个新的从头变异，c.142G > T . p.Phe48Val改变。所有的预测算法都预测这种变异是有害的。SNAP25是可溶性n -乙基马来酰亚胺敏感因子附着蛋白受体(SNARE)蛋白复合物的一部分，参与神经递质的胞外释放。动物模型中Snap25基因的改变会导致焦虑相关行为、共济失调和癫痫发作。我们认为，人类SNAP25突变是智力残疾和癫痫的一种新的遗传原因。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Rare diseases (Austin, Tex.)

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