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心肌衰老与细胞衰老:干细胞何去何从?

Myocardial aging and senescence: where have the stem cells gone?

作者信息

Sussman Mark A, Anversa Piero

机构信息

SDSU Heart Institute, San Diego State University, Department of Biology, LS426, San Diego, California 98182, USA.

出版信息

Annu Rev Physiol. 2004;66:29-48. doi: 10.1146/annurev.physiol.66.032102.140723.

Abstract

Heart failure remains a leading cause of hospital admissions and mortality in the elderly, and current interventional approaches often fail to treat the underlying cause of pathogenesis. Preservation of structure and function in the aging myocardium is most likely to be successful via ongoing cellular repair and replacement, as well as survival of existing cardiomyocytes that generate contractile force. Research has led to a paradigm shift driven by application of stem cells to generate cardiovascular cell lineages. Early controversial findings of pluripotent precursors adopting cardiac phenotypes are now widely accepted, and current debate centers upon the efficiency of progenitor cell incorporation into the myocardium. Much work remains to be done in determining the relevant progenitor cell population and optimizing conditions for efficient differentiation and integration. Significant implications exist for treatment of pathologically damaged or aging myocardium since future interventional approaches will capitalize upon the use of cardiac stem cells as therapeutic reagents.

摘要

心力衰竭仍然是老年人住院和死亡的主要原因,而目前的介入方法往往无法治疗发病机制的根本原因。通过持续的细胞修复和替换,以及产生收缩力的现有心肌细胞的存活,衰老心肌中的结构和功能保存最有可能成功。研究导致了一种范式转变,这是由应用干细胞产生心血管细胞谱系驱动的。多能前体细胞呈现心脏表型这一早期有争议的发现现在已被广泛接受,而目前的争论集中在祖细胞整合到心肌中的效率上。在确定相关的祖细胞群体以及优化有效分化和整合的条件方面,仍有许多工作要做。由于未来的介入方法将利用心脏干细胞作为治疗试剂,因此对病理受损或衰老心肌的治疗具有重大意义。

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