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Genetic and Physiologic Dissection of the Vertebrate Cardiac Conduction System

机译:椎体心脏传导系统的遗传和生理解剖

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摘要

Vertebrate hearts depend on highly specialized cardiomyocytes that form the cardiac conduction system (CCS) to coordinate chamber contraction and drive blood efficiently and unidirectionally throughout the organism. Defects in this specialized wiring system can lead to syncope and sudden cardiac death. Thus, a greater understanding of cardiac conduction development may help to prevent these devastating clinical outcomes. Utilizing a cardiac-specific fluorescent calcium indicator zebrafish transgenic line, Tg(cmlc2:gCaMP)s878, that allows for in vivo optical mapping analysis in intact animals, we identified and analyzed four distinct stages of cardiac conduction development that correspond to cellular and anatomical changes of the developing heart. Additionally, we observed that epigenetic factors, such as hemodynamic flow and contraction, regulate the fast conduction network of this specialized electrical system. To identify novel regulators of the CCS, we designed and performed a new, physiology-based, forward genetic screen and identified for the first time, to our knowledge, 17 conduction-specific mutations. Positional cloning of hobgoblins634 revealed that tcf2, a homeobox transcription factor gene involved in mature onset diabetes of the young and familial glomerulocystic kidney disease, also regulates conduction between the atrium and the ventricle. The combination of the Tg(cmlc2:gCaMP)s878 line/in vivo optical mapping technique and characterization of cardiac conduction mutants provides a novel multidisciplinary approach to further understand the molecular determinants of the vertebrate CCS.
机译:脊椎动物的心脏依赖于形成心脏传导系统(CCS)的高度专业化的心肌细胞,以协调腔室收缩并在整个生物体内高效单向驱动血液。此专用接线系统中的缺陷可能导致晕厥和心脏猝死。因此,对心脏传导发育的更多了解可能有助于预防这些破坏性的临床结果。利用心脏特异性荧光钙指示剂斑马鱼转基因品系Tg(cmlc2:gCaMP)s878,可以对完整动物进行体内光学作图分析,我们确定并分析了与细胞和解剖学变化相对应的心脏传导发育的四个不同阶段不断发展的心脏。此外,我们观察到表观遗传因素,例如血液动力流动和收缩,调节了该专门电气系统的快速传导网络。为了确定CCS的新型调节剂,我们设计并进行了基于生理的新的正向遗传筛选,并据我们所知首次确定了17种传导特异性突变。 Hobgoblins634的位置克隆显示,tcf2是一种与年轻和家族性肾小球囊性肾病的成熟发病糖尿病有关的同源盒转录因子基因,它也调节心房和心室之间的传导。 Tg(cmlc2:gCaMP)s878线/体内光学作图技术与心脏传导突变体特征的结合提供了一种新颖的多学科方法,可以进一步了解脊椎动物CCS的分子决定因素。

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