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构建心房的心肌细胞增殖动力学的多色映射。

Multicolor mapping of the cardiomyocyte proliferation dynamics that construct the atrium.

作者信息

Foglia Matthew J, Cao Jingli, Tornini Valerie A, Poss Kenneth D

机构信息

Department of Cell Biology, Duke University School of Medicine, Durham, NC 27710, USA.

Department of Cell Biology, Duke University School of Medicine, Durham, NC 27710, USA

出版信息

Development. 2016 May 15;143(10):1688-96. doi: 10.1242/dev.136606. Epub 2016 Mar 17.

Abstract

The orchestrated division of cardiomyocytes assembles heart chambers of distinct morphology. To understand the structural divergence of the cardiac chambers, we determined the contributions of individual embryonic cardiomyocytes to the atrium in zebrafish by multicolor fate-mapping and we compare our analysis to the established proliferation dynamics of ventricular cardiomyocytes. We find that most atrial cardiomyocytes become rod-shaped in the second week of life, generating a single-muscle-cell-thick myocardial wall with a striking webbed morphology. Inner pectinate myofibers form mainly by direct branching, unlike delamination events that create ventricular trabeculae. Thus, muscle clones assembling the atrial chamber can extend from wall to lumen. As zebrafish mature, atrial wall cardiomyocytes proliferate laterally to generate cohesive patches of diverse shapes and sizes, frequently with dominant clones that comprise 20-30% of the wall area. A subpopulation of cardiomyocytes that transiently express atrial myosin heavy chain (amhc) contributes substantially to specific regions of the ventricle, suggesting an unappreciated level of plasticity during chamber formation. Our findings reveal proliferation dynamics and fate decisions of cardiomyocytes that produce the distinct architecture of the atrium.

摘要

心肌细胞的有序分裂组装成形态各异的心脏腔室。为了解心脏腔室的结构差异,我们通过多色命运图谱确定了斑马鱼个体胚胎心肌细胞对心房的贡献,并将我们的分析与已确定的心室心肌细胞增殖动态进行比较。我们发现,大多数心房心肌细胞在出生后第二周变成杆状,形成一层单肌细胞厚的心肌壁,具有明显的网状形态。内部梳状肌纤维主要通过直接分支形成,这与形成心室小梁的分层事件不同。因此,组装心房腔室的肌肉克隆可以从壁延伸到腔。随着斑马鱼成熟,心房壁心肌细胞横向增殖,产生各种形状和大小的连贯斑块,通常有占壁面积20%-30%的优势克隆。短暂表达心房肌球蛋白重链(amhc)的心肌细胞亚群对心室的特定区域有很大贡献,这表明在腔室形成过程中存在未被认识到的可塑性水平。我们的研究结果揭示了产生心房独特结构的心肌细胞的增殖动态和命运决定。

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