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CCDC88C variants are associated with focal epilepsy and genotype–phenotype correlation

错义突变 癫痫 表型 生物 遗传学 外显子组测序 基因型 基因 神经科学
作者
Yujie Chen,Wenjie Wang,Dongfang Zou,Jianyuan Luo,Pengfei Jin,Liang Jin,Xiaorong Liu,Wei‐Ping Liao,Bin Li,Y. Chen
出处
期刊:Clinical Genetics [Wiley]
卷期号:105 (4): 397-405
标识
DOI:10.1111/cge.14476
摘要

CCDC88C gene, which encodes coiled-coil domain containing 88C, is essential for cell communication during neural development. Variants in the CCDC88C caused congenital hydrocephalus, some accompanied by seizures. In patients with epilepsy without acquired etiologies, we performed whole-exome sequencing (trio-based). Two de novo and two biallelic CCDC88C variants were identified in four cases with focal (partial) epilepsy. These variants did not present or had low frequencies in the gnomAD populations and were predicted to be damaging by multiple computational algorithms. Patients with de novo variants presented with adult-onset epilepsy, whereas patients with biallelic variants displayed infant-onset epilepsy. They all responded well to anti-seizure medications and were seizure-free. Further analysis showed that de novo variants were located at crucial domains, whereas one paired biallelic variants were located outside the crucial domains, and the other paired variant had a non-classical splicing and a variant located at crucial domain, suggesting a sub-molecular effect. CCDC88C variants associated with congenital hydrocephalus were all truncated, whereas epilepsy-associated variants were mainly missense, the proportion of which was significantly higher than that of congenital hydrocephalus-associated variants. CCDC88C is potentially associated with focal epilepsy with favorable outcome. The underlying mechanisms of phenotypic variation may correlation between genotype and phenotype.
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