TheSCN1AMutation Database: Updating Information and Analysis of the Relationships among Genotype, Functional Alteration, and Phenotype

错义突变 外显率 单倍率不足 生物 遗传学 表型 突变 基因型 基因 基因型-表型区分
作者
Heng Meng,Haiqing Xu,Lu Yu,Guo‐Wang Lin,Na He,Tao Su,Yi‐Wu Shi,Bin Li,Jie Wang,Xiao‐Rong Liu,Bin Tang,Yue‐Sheng Long,Yong‐Hong Yi,Wei‐Ping Liao
出处
期刊:Human Mutation [Wiley]
卷期号:36 (6): 573-580 被引量:207
标识
DOI:10.1002/humu.22782
摘要

Mutations in the SCN1A gene have been identified in epilepsy patients with widely variable phenotypes and modes of inheritance and in asymptomatic carriers. This raises challenges in evaluating the pathogenicity of SCN1A mutations. We systematically reviewed all SCN1A mutations and established a database containing information on functional alterations. In total, 1,257 mutations have been identified, of which 81.8% were not recurrent. There was a negative correlation between phenotype severity and missense mutation frequency. Further analyses suggested close relationships among genotype, functional alteration, and phenotype. Missense mutations located in different sodium channel regions were associated with distinct functional changes. Missense mutations in the pore region were characterized by the complete loss of function, similar to haploinsufficiency. Mutations with severe phenotypes were more frequently located in the pore region, suggesting that functional alterations are critical in evaluating pathogenicity and can be applied to patient management. A negative correlation was found between phenotype severity and familial incidence, and incomplete penetrance was associated with missense and splice site mutations, but not truncations or genomic rearrangements, suggesting clinical genetic counseling applications. Mosaic mutations with a load of 12.5-25.0% were potentially pathogenic with low penetrance, suggesting the need for future studies on less pathogenic genomic variations.
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