A novel deletion-frameshift mutation in the S1 region of HERG gene in a Chinese family with long QT syndrome 被引量：1

A novel deletion-frameshift mutation in the S1 region of HERG gene in a Chinese family with long QT syndrome

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摘要 Background The congenital Long QT syndrome （LQTS） is a hereditary cardiac channelopathy that is characterized by a prolonged QT interval,syncope,ventricular arrhythmias,and sudden death.The chromosome 7-linked type 2 congenital LQTS （LQT2） is caused by gene mutations in the human ether-a-go-go-related gene （HERG）.Methods A Chinese family diagnosed with LQTS were screened for KCNQ1,HERG and SCN5A,using polymerase chain reaction （PCR）,direct sequencing,and clong sequencing.We also investigated the mRNA expression of the HERG gene.Results We identified a novel i414fs＋98X mutation in the HERG gene.The deletion mutation of 14-bp in the first transmembrane segment （S1） introduced premature termination codons （PTCs） at the end of exon 6.This mutation would result in a serious phenotype if the truncated proteins co-assembled with normal subunit to form the defective channels.But only the proband was symptomatic.Conclusions We found that the mRNA level of the HERG gene was significantly lower in 1414fs＋98X carriers than in noncarriers.We found a novel 1414fs＋98X mutation.The mRNA level supports that NMD mechanism might regulate the novel mutation. Background The congenital Long QT syndrome （LQTS） is a hereditary cardiac channelopathy that is characterized by a prolonged QT interval,syncope,ventricular arrhythmias,and sudden death.The chromosome 7-linked type 2 congenital LQTS （LQT2） is caused by gene mutations in the human ether-a-go-go-related gene （HERG）.Methods A Chinese family diagnosed with LQTS were screened for KCNQ1,HERG and SCN5A,using polymerase chain reaction （PCR）,direct sequencing,and clong sequencing.We also investigated the mRNA expression of the HERG gene.Results We identified a novel i414fs＋98X mutation in the HERG gene.The deletion mutation of 14-bp in the first transmembrane segment （S1） introduced premature termination codons （PTCs） at the end of exon 6.This mutation would result in a serious phenotype if the truncated proteins co-assembled with normal subunit to form the defective channels.But only the proband was symptomatic.Conclusions We found that the mRNA level of the HERG gene was significantly lower in 1414fs＋98X carriers than in noncarriers.We found a novel 1414fs＋98X mutation.The mRNA level supports that NMD mechanism might regulate the novel mutation.

作者 GAO Ying ZHANG Ping LI Xue-bin WU Cun-cao GUO Ji-hong

机构地区 Department of Cardiac Electrophysiology

出处《Chinese Medical Journal》 SCIE CAS CSCD 2013年第16期3093-3096,共4页 中华医学杂志（英文版）

关键词 deletion mutation HERG inherited arrhythmia Long QT syndrome nonsense mediated decay deletion mutation HERG inherited arrhythmia Long QT syndrome nonsense mediated decay

分类号 Q463 [生物学—生理学] Q513 [生物学—生物化学]

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2013年第16期

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A novel deletion-frameshift mutation in the S1 region of HERG gene in a Chinese family with long QT syndrome 被引量：1

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