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作 者:黄艳[1] 刘光华[2] 王世彪[2] 刘晖[2] 周有峰[2] Huang Yan;Liu Guanghua;Wang Shibiao;Liu Hui;Zhou Youfeng(Department of Children’s Healthcare,Fujian Provincial Maternity and Children’s Hospital,the Affiliated Hospital of Fujian Medical University,Fuzhou,Fujian 350001,China;Department of Pediatrics,Fujian Provincial Maternity and Children’s Hospital,the Affiliated Hospital of Fujian Medical University,Fuzhou,Fujian 350001,China)
机构地区:[1]福建省妇幼保健院儿童保健科,福建医科大学附属医院,福州350001 [2]福建省妇幼保健院儿科,福建医科大学附属医院,福州350001
出 处:《中华医学遗传学杂志》2020年第4期479-482,共4页Chinese Journal of Medical Genetics
摘 要:目的对一例疑诊Menkes病患儿进行临床和遗传学分析。方法提取患儿及其父母基因组DNA,行家系全外显子测序及多重连接探针扩增技术检测ATP7A基因微重复、缺失,对疑似致病变异行生物信息学分析,并对患儿及其父母行一代测序验证变异位点。结果在受检者ATP7A基因发现c.1870-13T>G的核苷酸变异,为新发剪切变异。结论该患儿为ATP7A基因c.1870-13T>G变异而导致Menkes病,家系全外显子测序为表型异质性强的遗传性疾病提供了有力工具。Objective To carry out genetic testing for a male infant suspected for Menkes disease.Methods Genomic DNA of the proband and his parents were extracted and subjected to family trio whole-exome sequencing(WES).Microduplication and microdeletion of the ATP7A gene were detected by multiplex ligation-dependent probe amplification(MLPA).Suspected variants were subjected to bioinformatic analysis and verified by Sanger sequencing.Results The proband was found to harbor a de novo c.1870-13T>G variation of the ATP7A gene,which may alter a splice site and affect its protein product.Conclusion The patient was diagnosed with Menkes disease due to the c.1870-13T>G variant of the ATP7A gene.Whole-exome sequencing of family trios is a powerful tool for the diagnosis of diseases with strong phenotypic heterogeneity.
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