Novel Variants of CEP152 in a Case of Compound-Heterozygous Inheritance of Epilepsy.

IF 1.2 Q4 GENETICS & HEREDITY Global Medical Genetics Pub Date : 2024-01-16 eCollection Date: 2024-01-01 DOI:10.1055/s-0043-1777807
Weiran Li, Xiaowei Lu, Jianbo Shu, Yingzi Cai, Dong Li, Chunquan Cai
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Abstract

IntroductionCEP152 encodes protein Cep152, which associates with centrosome function. The lack of Cep152 can cause centrosome duplication to fail. CEP152 mutates, causing several diseases such as Seckel syndrome-5 and primary microencephaly-9. Methods  In this study, we reported a patient diagnosed with epilepsy in Tianjin Children's Hospital. We performed clinical examination and laboratory test, and whole-exome sequencing was performed for the proband's and his parents' peripheral blood. The suspected compound-heterozygous variant in the CEP152 gene was verified by Sanger sequencing and quantitative real-time polymerase chain reaction technology. Results  We discovered three variants-two of them from CEP152 and one from HPD . The result showed the variants in CEP152 only. The patient presented with seizures frequently. Sanger sequencing showed two novel variants in CEP152 are in exon26 (NM_014985.3 c.3968C > A p.Ser1323*) and in exon16 (NM_014985.3 c.2034_2036del p.Tyr678*). Conclusions  We reported a novel compound-heterozygous variant in the CEP152 gene in this study. Most of the phenotypes are Seckel syndrome and primary microencephaly, and the novel variant may cause an atypical phenotype that is epilepsy.

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一例复合杂合子癫痫遗传中的 CEP152 新变体
引言 CEP152编码与中心体功能有关的蛋白质Cep152。缺乏 Cep152 会导致中心体复制失败。CEP152 基因突变可导致多种疾病,如塞克尔综合征(Seckel Syndrome-5)和原发性小脑症(primary microencephaly-9)。方法 本研究报告了天津市儿童医院的一名癫痫患者。我们对患者进行了临床检查和实验室检测,并对患者及其父母的外周血进行了全基因组测序。通过桑格测序和定量实时聚合酶链式反应技术对疑似的 CEP152 基因复合杂合变异进行了验证。结果 我们发现了三个变体,其中两个来自 CEP152,一个来自 HPD。结果显示只有 CEP152 存在变异。患者经常出现癫痫发作。桑格测序显示,CEP152 的两个新型变异位于外显子 26 (NM_014985.3 c.3968C > A p.Ser1323*) 和外显子 16 (NM_014985.3 c.2034_2036del p.Tyr678*)。结论 本研究报告了一种新型的 CEP152 基因复合杂合子变异。大多数表型为塞克尔综合征和原发性小脑畸形,而该新型变异可能导致非典型表型,即癫痫。
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来源期刊
Global Medical Genetics
Global Medical Genetics GENETICS & HEREDITY-
自引率
11.80%
发文量
30
审稿时长
14 weeks
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