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Nuclear and Chromatin Reorganization during Cell Senescence and Aging – A Mini-Review

机译:细胞衰老和衰老过程中的核和染色质重组–综述

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摘要

Genetic material in the nucleus governs mechanisms related to cell proliferation, differentiation, and function. Thus, senescence and aging are directly tied to the change of nuclear function and structure. The most important mechanisms that affect cell senescence are: (i) telomere shortening; (ii) environmental stress-mediated accumulation of DNA mutations, and (iii) the intrinsically encoded biological clock that dictates lifespan events of any particular cell type. Overall, these changes lead to modification of the expression of genes that are responsible for: (i) organization of the nuclear structure; (ii) integrity of transcriptionally inactive heterochromatin, and (iii) epigenetic modification of chromosomes due to DNA methylation and/or histone modifications. These aging-related nuclear alterations do not only affect somatic cells. More importantly, they affect stem cells, which are responsible for proper tissue rejuvenation. In this review, we focus on epigenetic changes in the chromatin structure and their impact on the biology and function of adult cells as they age. We will also address aging-related changes in a compartment of the most primitive pluripotent stem cells that were recently identified by our team and named ‘very small embryonic/epiblast-like stem cells’.
机译:细胞核中的遗传物质控制着与细胞增殖,分化和功能有关的机制。因此,衰老和衰老与核功能和结构的变化直接相关。影响细胞衰老的最重要机制是:(i)端粒缩短; (ii)环境胁迫介导的DNA突变积累,以及(iii)内在编码的生物钟,指示任何特定细胞类型的寿命事件。总的来说,这些变化导致基因表达的修饰,这些基因负责:(i)核结构的组织; (ii)转录失活的异染色质的完整性,和(iii)由于DNA甲基化和/或组蛋白修饰而引起的染色体表观遗传修饰。这些与衰老相关的核变化不仅影响体细胞。更重要的是,它们影响干细胞,这些干细胞负责适当的组织再生。在这篇综述中,我们关注染色质结构的表观遗传学变化及其对成年细胞随着年龄增长的生物学和功能的影响。我们还将解决最原始的多能干细胞隔室中与衰老有关的变化,这些变化最近被我们的研究小组发现,并被称为“非常小的胚胎/上皮样干细胞”。

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