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流入道中平滑肌细胞的心脏起源。

Cardiac origin of smooth muscle cells in the inflow tract.

机构信息

Department of Molecular Cell and Developmental Biology, University of California, Los Angeles, Los Angeles, CA 90095, USA.

出版信息

J Mol Cell Cardiol. 2011 Feb;50(2):337-45. doi: 10.1016/j.yjmcc.2010.10.009. Epub 2010 Oct 23.

Abstract

Multipotent Isl1(+) heart progenitors give rise to three major cardiovascular cell types: cardiac, smooth muscle, and endothelial cells, and play a pivotal role in lineage diversification during cardiogenesis. A critical question is pinpointing when this cardiac-vascular lineage decision is made, and how this plasticity serves to coordinate cardiac chamber and vessel growth. The posterior domain of the Isl1-positive second heart field contributes to the SLN-positive atrial myocardium and myocardial sleeves in the cardiac inflow tract, where myocardial and vascular smooth muscle layers form anatomical and functional continuity. Herein, using a new atrial specific SLN-Cre knockin mouse line, we report that bipotent Isl1(+)/SLN(+) transient cell population contributes to cardiac as well as smooth muscle cells at the heart-vessel junction in cardiac inflow tract. The Isl1(+)/SLN(+) cells are capable of giving rise to cardiac and smooth muscle cells until late gestational stages. These data suggest that the cardiac and smooth muscle cells in the cardiac inflow tract share a common developmental origin. This article is part of a special issue entitled, "Cardiovascular Stem Cells Revisited".

摘要

多能性 Isl1(+)心脏祖细胞分化为三种主要的心血管细胞类型:心肌细胞、平滑肌细胞和内皮细胞,并在心脏发生过程中的谱系多样化中发挥关键作用。一个关键问题是确定何时做出这种心脏-血管谱系决定,以及这种可塑性如何协调心脏腔室和血管的生长。Isl1 阳性的第二心脏场的后域有助于 SLN 阳性的心房心肌和心腔流入道中的心肌袖,其中心肌和血管平滑肌层形成解剖和功能连续性。在此,我们使用一种新的心房特异性 SLN-Cre 敲入小鼠系,报告双能 Isl1(+)/SLN(+)瞬态细胞群有助于心腔流入道中心血管交界处的心肌和平滑肌细胞。Isl1(+)/SLN(+)细胞能够产生心肌和平滑肌细胞,直到妊娠晚期。这些数据表明,心腔流入道中的心肌和平滑肌细胞具有共同的发育起源。本文是题为“心血管干细胞再探”的特刊的一部分。

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Cardiac origin of smooth muscle cells in the inflow tract.流入道中平滑肌细胞的心脏起源。
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