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探讨表观遗传学及其与肌肉和骨骼衰老的关系。

A review of epigenetics and its association with ageing of muscle and bone.

机构信息

MRC Lifecourse Epidemiology Centre, University of Southampton, SO16 6YD, United Kingdom of Great Britain and Northern Ireland.

MRC Lifecourse Epidemiology Centre, University of Southampton, SO16 6YD, United Kingdom of Great Britain and Northern Ireland.

出版信息

Maturitas. 2022 Nov;165:12-17. doi: 10.1016/j.maturitas.2022.06.014. Epub 2022 Jul 11.

DOI:10.1016/j.maturitas.2022.06.014
PMID:35841774
Abstract

Ageing is defined as the 'increasing frailty of an organism with time that reduces the ability of that organism to deal with stress'. It has been suggested that epigenetics may underlie the observation that some individuals appear to age faster than others. Epigenetics is the study of changes which occur in an organism due to changes in expression of the genetic code rather than changes to the genetic code itself; that is, epigenetic mechanisms impact upon the function of DNA without changing the DNA sequence. It is important to recognise that epigenetic changes, in contrast to genetic changes, can vary according to different cell types and therefore can demonstrate significant tissue-specificity. There are different types of epigenetic mechanisms: histone modification, non-coding RNAs and DNA methylation. Epigenetic clocks have been developed using statistical techniques to identify the optimal combination of CpG sites (from methylation arrays) to correlate with chronological age. This review considers how epigenetic factors may affect rates of ageing of muscle and bone and provides an overview of current understanding in this area. We discuss studies using first-generation epigenetic clocks, as well as the second-generation iterations, which appear to show stronger associations with the ageing muscle phenotype. We also review epigenome-wide association studies that have been performed in various tissues examining relationships with osteoporosis and fracture. It is hoped that an understanding of this area will lead to interventions that might prevent or reduce rates of musculoskeletal ageing in later life.

摘要

衰老是指“随着时间的推移,生物体的脆弱性逐渐增加,从而降低了生物体应对压力的能力”。有人认为,表观遗传学可能是导致一些人看起来比其他人衰老得更快的原因。表观遗传学是研究由于遗传密码表达的变化而不是遗传密码本身的变化而在生物体中发生的变化;也就是说,表观遗传机制影响 DNA 的功能而不改变 DNA 序列。重要的是要认识到,与遗传变化相比,表观遗传变化可以根据不同的细胞类型而有所不同,因此可以表现出显著的组织特异性。有不同类型的表观遗传机制:组蛋白修饰、非编码 RNA 和 DNA 甲基化。表观遗传钟是使用统计技术开发的,用于识别与年龄相关的最佳 CpG 位点组合(来自甲基化阵列)。这篇综述考虑了表观遗传因素如何影响肌肉和骨骼的衰老速度,并概述了这一领域的现有认识。我们讨论了使用第一代表观遗传钟的研究,以及第二代迭代,它们似乎与衰老的肌肉表型有更强的关联。我们还回顾了在不同组织中进行的全基因组关联研究,这些研究检查了与骨质疏松症和骨折的关系。希望对这一领域的了解将导致能够预防或减少晚年肌肉骨骼衰老速度的干预措施。

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