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首页> 外文期刊>Epilepsy & behavior: E&B >A case of autosomal dominant nocturnal frontal lobe epilepsy (ADNFLE) coexisting with pervasive developmental disorder harboring SCN1A mutation in addition to CHRNB2 mutation
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A case of autosomal dominant nocturnal frontal lobe epilepsy (ADNFLE) coexisting with pervasive developmental disorder harboring SCN1A mutation in addition to CHRNB2 mutation

机译:一例常染色体显性遗传性夜额叶癫痫(ADNFLE)与CHRNB2突变之外还携带SCN1A突变的普遍性发育障碍并存

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摘要

We report a case of autosomal dominant nocturnal frontal lobe epilepsy (ADNFLE) with several characteristics distinct from previously reported cases, in which genetic studies identified mutations in two different genes. This case differed from typical ADNFLE with respect to the following: (1) slightly younger onset and refractory to antiepileptic drugs and (2) borderline intellectual functioning and coexistence of pervasive developmental disorder from infancy. Genetic testing revealed a novel mutation and a silent substitution in SCN1A (c.4285G. >. T, A1429S and c.4371G. > C, silent) in addition to a known mutation in CHRNB2 (c.1200C. > G, I312M). SCN1A is a gene that codes for the voltage-dependent sodium channel α1 subunit and has been implicated in generalized epilepsy with febrile seizures plus and severe myoclonic epilepsy in infancy. However, the relation between SCN1A and ADNFLE is unknown. We report the clinical course and symptomatic characteristics of this case although the relationship between ADNFLE mutation and SCN1A mutation remains to be elucidated.
机译:我们报告一例常染色体显性遗传性夜额叶癫痫(ADNFLE),其特征与以前报道的病例不同,其中遗传研究确定了两个不同基因的突变。该病例在以下方面与典型的ADNFLE不同:(1)发病年龄稍小,抗癫痫药难治;(2)边缘性智力功能和婴儿期普遍存在的发育障碍并存。遗传测试显示,除​​了CHRNB2的已知突变(c.1200C。> G,I312M)之外,SCN1A(c.4285G。>。T,A1429S和c.4371G。> C,沉默)中也出现了新的突变和沉默取代。 。 SCN1A是一个编码电压依赖性钠通道α1亚基的基因,与婴儿期高热性癫痫发作加重度肌阵挛性癫痫有关。但是,SCN1A和ADNFLE之间的关系是未知的。尽管ADNFLE突变和SCN1A突变之间的关系仍有待阐明,但我们报告了此病例的临床过程和症状特征。

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