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首页> 外文期刊>Molecular Genetics & Genomic Medicine >Mutations in the PH Domain of DNM1 are associated with a nonepileptic phenotype characterized by developmental delay and neurobehavioral abnormalities
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Mutations in the PH Domain of DNM1 are associated with a nonepileptic phenotype characterized by developmental delay and neurobehavioral abnormalities

机译:DNM1的PH结构域中的突变与一种以发育迟缓和神经行为异常为特征的非癫痫性表型有关

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Background Dynamin 1 is a protein involved in the synaptic vesicle cycle, which facilitates the exocytosis of neurotransmitters necessary for normal signaling and development in the central nervous system. Pathogenic variants in DNM1 have been implicated in global developmental delay (DD), severe intellectual disability (ID), and notably, epileptic encephalopathy. All previously reported DNM1 pathogenic variants causing this severe phenotype occur in the GTPase and Middle domains of the dynamin 1 protein. Methods We used whole‐exome sequencing to characterize the molecular basis of DD and autistic symptoms in two identical siblings. Results The twin siblings exhibit mild to moderate ID and autistic symptoms but no epileptic encephalopathy. Exome sequencing revealed a genetic variant, c.1603AG (p.Lys535Glu), in the PH domain of dynamin 1. Previous in?vitro studies showed that mutations at Lys535 inhibit endocytosis and impair PH loop binding to PIP2. Conclusions Our data suggest a previously undescribed milder phenotype associated with a missense genetic variant in the PH domain of dynamin 1.
机译:背景动力蛋白1是一种参与突触小泡循环的蛋白质,其促进中枢神经系统正常信号传导和发育所必需的神经递质的胞吐作用。 DNM1的致病变异与全球发育延迟(DD),严重智力障碍(ID)以及癫痫性脑病有关。导致此严重表型的所有先前报道的DNM1致病变体都发生在发电机1蛋白的GTPase和中间结构域中。方法我们使用全外显子组测序来表征两个相同兄弟姐妹中DD和自闭症症状的分子基础。结果双胞胎兄弟姐妹表现出轻度至中度的内ID和自闭症状,但没有癫痫性脑病。外显子组测序揭示了在dynamin 1的PH域中有一个遗传变异,c.1603A> G(p.Lys535Glu)。先前的体外研究表明,Lys535处的突变抑制内吞作用并损害PH环与PIP2的结合。结论我们的数据表明,以前未描述的较温和的表型与动力蛋白1 PH域中的错义遗传变异有关。

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