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Identification of genetic causes in children with unexplained epilepsy based on trio‐whole exome sequencing

外显子组测序 癫痫 外显子组 癫痫综合征 基因检测 遗传咨询 遗传学 医学 染色体 遗传分析 拷贝数变化 基因型 儿科 生物 表型 生物信息学 基因 精神科 基因组
作者
Chengyan Li,Xue Chupeng,You Wang,Chen Yinhui,Huang Binglong,Ao Dang,Ling Liu,Chuan Tian
出处
期刊:Clinical Genetics [Wiley]
卷期号:106 (2): 140-149 被引量:4
标识
DOI:10.1111/cge.14519
摘要

Genotype and clinical phenotype analyses of 128 children were performed based on whole exome sequencing (WES), providing a reference for the provision of genetic counseling and the precise diagnosis and treatment of epilepsy. A total of 128 children with unexplained epilepsy were included in this study, and all their clinical data were analyzed. The children's treatments, epilepsy control, and neurodevelopmental levels were regularly followed up every 3 months. The genetic diagnostic yield of the 128 children with epilepsy is 50.8%, with an SNV diagnostic yield of 39.8% and a CNV diagnostic yield of 12.5%. Among the 128 children with epilepsy, 57.0% had onset of epilepsy in infancy, 25.8% have more than two clinical seizure forms, 62.5% require two or more anti-epileptic drug treatments, and 72.7% of the children have varying degrees of psychomotor development retardation. There are significant differences between ages of onset, neurodevelopmental levels and the presence of drug resistance in the genetic diagnostic yield (all p < 0.05). The 52 pathogenic/likely pathogenic SNVs involve 31 genes, with genes encoding ion channels having the largest number of mutations (30.8%). There were 16 cases of pathogenic/possibly pathogenic CNVs, among which the main proportions of CNVs were located in chromosome 15 and chromosome 16. Trio-WES is an essential tool for the genetic diagnosis of unexplained epilepsy, with a genetic diagnostic yield of up to 50.8%. Early genetic testing can provide an initiate appropriate therapies and accurate molecular diagnosis.
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