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成年蝾螈再生心肌细胞的异质性增殖潜能。

Heterogeneous proliferative potential in regenerative adult newt cardiomyocytes.

作者信息

Bettencourt-Dias Monica, Mittnacht Sybille, Brockes Jeremy P

机构信息

Department of Biochemistry, University College London, London WC1E 6BT, UK.

出版信息

J Cell Sci. 2003 Oct 1;116(Pt 19):4001-9. doi: 10.1242/jcs.00698. Epub 2003 Aug 19.

DOI:10.1242/jcs.00698
PMID:12928330
Abstract

Adult newt cardiomyocytes, in contrast to their mammalian counterparts, can proliferate after injury and contribute to the functional regeneration of the heart. In order to understand the mechanisms underlying this plasticity we performed longitudinal studies on single cardiomyocytes in culture. We find that the majority of cardiomyocytes can enter S phase, a process that occurs in response to serum-activated pathways and is dependent on the phosphorylation of the retinoblastoma protein. However, more than half of these cells stably arrest at either entry to mitosis or during cytokinesis, thus resembling the behaviour observed in mammalian cardiomyocytes. Approximately a third of the cells progress through mitosis and may enter successive cell divisions. When cardiomyocytes divided more than once, the proliferative behaviour of sister cells was significantly correlated, in terms of whether they underwent a subsequent cell cycle, and if so, the duration of that cycle. These observations suggest a mechanism whereby newt heart regeneration depends on the retention of proliferative potential in a subset of cardiomyocytes. The regulation of the remaining newt cardiomyocytes is similar to that described for their mammalian counterparts, as they arrest during mitosis or cytokinesis. Understanding the nature of this block and why it arises in some but not other newt cardiomyocytes may lead to an augmentation of the regenerative potential in the mammalian heart.

摘要

与哺乳动物的成年心肌细胞不同,成年蝾螈心肌细胞在损伤后能够增殖,并有助于心脏的功能再生。为了了解这种可塑性背后的机制,我们对培养中的单个心肌细胞进行了纵向研究。我们发现,大多数心肌细胞能够进入S期,这一过程是对血清激活途径的反应,并且依赖于视网膜母细胞瘤蛋白的磷酸化。然而,这些细胞中有超过一半在进入有丝分裂或胞质分裂过程中稳定停滞,因此类似于在哺乳动物心肌细胞中观察到的行为。大约三分之一的细胞完成有丝分裂,并可能进入连续的细胞分裂。当心肌细胞进行多次分裂时,姐妹细胞的增殖行为在是否经历后续细胞周期以及如果经历,该周期的持续时间方面显著相关。这些观察结果提示了一种机制,即蝾螈心脏再生依赖于一部分心肌细胞增殖潜能的保留。其余蝾螈心肌细胞的调控与其哺乳动物对应物相似,因为它们在有丝分裂或胞质分裂过程中停滞。了解这种阻滞的本质以及为什么它在一些蝾螈心肌细胞中出现而在其他细胞中不出现,可能会增强哺乳动物心脏的再生潜能。

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