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Cardiac electrophysiology in genetically engineered mice.

机译:基因工程小鼠的心脏电生理。

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摘要

The mouse has become the principal animal model for studying biologic processes in mammals. Major advances in transgene and gene targeting technology enabled manipulation of the mouse genome in a predictable fashion. Mutant mouse strains provide important insights into the molecular mechanisms underlying normal and disordered cardiac conduction and sudden cardiac death. A variety of mouse strains harboring gene mutations leading to inherited developmental disorders have been designed. Structural protein abnormalities, connexin protein defects, and ion channelopathies associated with human clinical phenotypes, including congenital heart disease, cardiomyopathies, long QT syndrome, and muscular dystrophy, have been engineered into the mouse genome, creating models of human electrophysiologic disease. Functional analyses of the underlying molecular mechanisms of resultant phenotypes require appropriate and sophisticated experimental methodology. In this review, genetic mouse models pertinent to human arrhythmogenic disorders and their application to present-day ex vivo and in vivo murine electrophysiologic technology at the whole organ and animal levels are discussed.
机译:小鼠已成为研究哺乳动物生物学过程的主要动物模型。转基因和基因靶向技术的重大进步使小鼠基因组的操纵可预测的方式。突变的小鼠品系提供了对正常和异常心脏传导以及心脏猝死的分子机制的重要见解。已经设计了多种带有导致遗传性发育障碍的基因突变的小鼠品系。与人类临床表型相关的结构蛋白异常,连接蛋白缺陷和离子通道病变,包括先天性心脏病,心肌病,长QT综合征和肌营养不良症,已经被工程化到小鼠基因组中,从而创建了人类电生理疾病模型。结果表型的潜在分子机制的功能分析需要适当和复杂的实验方法。在这篇综述中,讨论了与人类心律失常性疾病有关的遗传小鼠模型及其在整个器官和动物水平上在当今离体和体内鼠电生理技术中的应用。

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