肌阵挛性癫痫
Dravet综合征
癫痫
错义突变
医学
儿科
突变
生物
生物信息学
遗传学
精神科
基因
作者
Lieve Claes,Berten Ceulemans,Dominique Audenaert,Katrien Smets,Ann Löfgren,Jurgen Del‐Favero,Sirpa Ala‐Mello,Lina Basel‐Vanagaite,Barbara Plecko,Salmo Raskin,Paul Thiry,Nicole I. Wolf,Christine Van Broeckhoven,Peter De Jonghe
出处
期刊:Human Mutation
[Wiley]
日期:2003-04-22
卷期号:21 (6): 615-621
被引量:201
摘要
Severe myoclonic epilepsy of infancy (SMEI or Dravet syndrome) is a rare disorder occurring in young children often without a family history of a similar disorder. The earliest disease manifestations are usually fever-associated seizures. Later in life, patients display different types of afebrile seizures including myoclonic seizures. Arrest of psychomotor development occurs in the second year of life and most patients become ataxic. Patients are resistant to antiepileptic drug therapy. Recently, we described de novo mutations of the neuronal sodium channel alpha-subunit gene SCN1A in seven isolated SMEI patients. To investigate the contribution of SCN1A mutations to the etiology of SMEI, we examined nine additional SMEI patients. We observed eight coding and one noncoding mutation. In contrast to our previous study, most mutations are missense mutations clustering in the S4-S6 region of SCN1A. These findings demonstrate that de novo mutations in SCN1A are a major cause of isolated SMEI.
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