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Genetics of congenital and drug-induced long QT syndromes: current evidence and future research perspectives

机译:先天性和药物性长QT综合征的遗传学:当前证据和未来研究前景

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摘要

The long QT syndrome (LQTS) is a condition characterized by abnormal prolongation of the QT interval with an associated risk of ventricular arrhythmias and sudden cardiac death. Congenital forms of LQTS arise due to rare and highly penetrant mutations that segregate in a Mendelian fashion. Over the years, multiple mutations in genes encoding ion channels and ion channel binding proteins have been reported to underlie congenital LQTS. Drugs are by far the most common cause of acquired forms of LQTS. Emerging evidence suggests that drug-induced LQTS also has a significant heritable component. However, the genetic substrate underlying drug-induced LQTS is presently largely unknown. In recent years, advances in next-generation sequencing technology and molecular biology techniques have significantly enhanced our ability to identify genetic variants underlying both monogenic diseases and more complex traits. In this review, we discuss the genetic basis of congenital and drug-induced LQTS and focus on future avenues of research in the field. Ultimately, a detailed characterization of the genetic substrate underlying congenital and drug-induced LQTS will enhance risk stratification and potentially result in the development of tailored genotype-based therapies.
机译:长QT综合征(LQTS)是一种以QT间期异常延长为特征的疾病,伴有室性心律失常和猝死的危险。 LQTS的先天形式是由于以孟德尔方式分离的罕见且高度渗透性的突变而产生的。多年来,已经报道了编码离子通道和离子通道结合蛋白的基因中的多个突变是先天性LQTS的基础。迄今为止,药物是导致获得性LQTS形式的最常见原因。新兴证据表明,药物诱导的LQTS也具有重要的遗传成分。然而,目前基本未知药物诱导的LQTS的遗传底物。近年来,下一代测序技术和分子生物学技术的进步显着增强了我们识别单基因疾病和更复杂特征的遗传变异的能力。在这篇综述中,我们讨论了先天性和药物诱导的LQTS的遗传基础,并将重点放在该领域的未来研究途径上。最终,对先天性和药物诱导的LQTS的遗传底物的详细表征将增强风险分层,并有可能导致开发基于基因型的定制疗法。

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