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生成更多心肌。

Making more heart muscle.

作者信息

van den Hoff Maurice J B, Kruithof Boudewijn P T, Moorman Antoon F M

机构信息

Molecular and Experimental Cardiology Group, Academic Medical Center, University of Amsterdam, Amsterdam, The Netherlands.

出版信息

Bioessays. 2004 Mar;26(3):248-61. doi: 10.1002/bies.20006.

Abstract

Postnatally, heart muscle cells almost completely lose their ability to divide, which makes their loss after trauma irreversible. Potential repair by cell grafting or mobilizing endogenous cells is of particular interest for possible treatments for heart disease, where the poor capacity for cardiomyocyte proliferation probably contributes to the irreversibility of heart failure. Knowledge of the molecular mechanisms that underly formation of heart muscle cells might provide opportunities to repair the diseased heart by induction of (trans) differentiation of endogenous or exogenous cells into heart muscle cells. We briefly review the molecular mechanisms involved in early development of the linear heart tube by differentiation of mesodermal cells into heart muscle cells. Because the initial heart tube does not comprise all the cardiac compartments present in the adult heart, heart muscle cells are added to the distal borders of the tube and within the tube. At both distal borders, mesodermal cell are recruited into the cardiac lineage and, within the heart tube, muscular septa are formed. In this review, the relative late additions of heart muscle cells to the linear heart tube are described and the potential underlying molecular mechanisms are discussed.

摘要

出生后,心肌细胞几乎完全丧失分裂能力,这使得创伤后心肌细胞的损失不可逆转。通过细胞移植或动员内源性细胞进行潜在修复对于心脏病的可能治疗尤为重要,因为心肌细胞增殖能力差可能导致心力衰竭的不可逆性。了解心肌细胞形成的分子机制可能为通过诱导内源性或外源性细胞(转)分化为心肌细胞来修复患病心脏提供机会。我们简要回顾了中胚层细胞分化为心肌细胞从而参与线性心管早期发育的分子机制。由于最初的心管并不包含成体心脏中所有的心脏腔室,心肌细胞会添加到心管的远端边界以及心管内部。在两个远端边界,中胚层细胞被招募进入心脏谱系,并且在心管内部形成肌肉隔膜。在这篇综述中,描述了心肌细胞相对较晚添加到线性心管的情况,并讨论了潜在的分子机制。

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