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从多能性到不同的心肌细胞亚型。

From pluripotency to distinct cardiomyocyte subtypes.

机构信息

1st Medical Department, University of Munich, Campus Grosshadern, Munich, Germany.

出版信息

Physiology (Bethesda). 2012 Jun;27(3):119-29. doi: 10.1152/physiol.00044.2011.

Abstract

Differentiated adult cardiomyocytes (CMs) lack significant regenerative potential, which is one reason why degenerative heart diseases are the leading cause of death in the western world. For future cardiac repair, stem cell-based therapeutic strategies may become alternatives to donor heart transplantation. The principle of reprogramming adult terminally differentiated cells (iPSC) had a major impact on stem cell biology. One can now generate autologous pluripotent cells that highly resemble embryonic stem cells (ESC) and that are ethically inoffensive as opposed to human ESC. Yet, due to genetic and epigenetic aberrations arising during the full reprogramming process, it is questionable whether iPSC will enter the clinic in the near future. Therefore, the recent achievement of directly reprogramming fibroblasts into cardiomyocytes via a milder approach, thereby avoiding an initial pluripotent state, may become of great importance. In addition, various clinical scenarios will depend on the availability of specific cardiac cellular subtypes, for which a first step was achieved via our own programming approach to achieve cardiovascular cell subtypes. In this review, we discuss recent progress in the cardiovascular stem cell field addressing the above mentioned aspects.

摘要

分化的成体心肌细胞(CM)缺乏显著的再生潜能,这也是退行性心脏疾病成为西方世界主要致死原因之一。为了未来的心脏修复,基于干细胞的治疗策略可能成为供体心脏移植的替代方法。重编程成年终末分化细胞(iPSC)的原理对干细胞生物学产生了重大影响。现在可以生成自体多能细胞,这些细胞高度类似于胚胎干细胞(ESC),并且与人类 ESC 相比在伦理上没有问题。然而,由于在完全重编程过程中出现的遗传和表观遗传异常,iPSC 是否会在不久的将来进入临床仍存在疑问。因此,最近通过一种更温和的方法直接将成纤维细胞重编程为心肌细胞的成就可能变得非常重要,因为这种方法避免了初始多能状态。此外,各种临床情况将取决于特定心脏细胞亚型的可用性,我们已经通过自己的编程方法实现了心血管细胞亚型的获得,从而迈出了第一步。在这篇综述中,我们讨论了心血管干细胞领域的最新进展,这些进展涉及到上述方面。

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