{"title":"[Postnatal epigenome-mediated aging control and global trends].","authors":"Motoshi Hayano","doi":"10.3143/geriatrics.61.1","DOIUrl":null,"url":null,"abstract":"<p><p>The epigenome can adequately regulate the on/off states of genes in response to external environmental factors and stress. In recent years, it has been observed that the epigenome, which is modulated through DNA methylation, histone modifications, and chromatin remodeling, changes with age. Alterations in the epigenome lead to the loss of cell-specific epigenome/identity, which in turn triggers a decline in tissue function. In mammals, postnatal epigenomic variations are not only caused by metabolic diseases, such as diabetes or DNA damage, but also by social stress and infectious diseases. Unlike Genome-Wide Association Studies (GWAS), dynamically changing epigenomes, along with their cellular roles, need to be established as objective biomarkers in conjunction with various biological signals, such as walking speed, brain waves, and clinical data. The biological age/aging clock, determined by methylated DNA, has attracted attention, and calorie restriction not only slows the progression of aging, but also seems to suppress it. However, as indicated by gene expression analysis in aging mice, aging is not a linear model, but is represented by nonlinear dynamic changes. Consequently, the development of experimental models and analytical methods that enhance temporal resolution through time-series analysis, tailored to spatial resolution, such as cell distribution and organ specificity, is progressing. Moreover, in recent years, in addition to anti-aging efforts targeting epigenomic variations, global attention has increasingly focused on research and development aimed at rejuvenating treatments, thus leading to the birth of many biotech companies. Aging Hallmarks such as inflammation, stem cells, metabolism, genomic instability, and autophagy, interact closely with the epigenome. Various postnatal and reversible epigenomic controls of aging, including Yamanaka factors (OKSM and OSK), are now entering a new phase. In the future, the development of aging control using diverse modalities, such as mRNA, artificial peptides, and genome editing, is expected, along with an improved molecular understanding of aging and identification of useful biomarkers.</p>","PeriodicalId":35593,"journal":{"name":"Japanese Journal of Geriatrics","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2024-01-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Japanese Journal of Geriatrics","FirstCategoryId":"1085","ListUrlMain":"https://doi.org/10.3143/geriatrics.61.1","RegionNum":0,"RegionCategory":null,"ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q4","JCRName":"Medicine","Score":null,"Total":0}
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Abstract
The epigenome can adequately regulate the on/off states of genes in response to external environmental factors and stress. In recent years, it has been observed that the epigenome, which is modulated through DNA methylation, histone modifications, and chromatin remodeling, changes with age. Alterations in the epigenome lead to the loss of cell-specific epigenome/identity, which in turn triggers a decline in tissue function. In mammals, postnatal epigenomic variations are not only caused by metabolic diseases, such as diabetes or DNA damage, but also by social stress and infectious diseases. Unlike Genome-Wide Association Studies (GWAS), dynamically changing epigenomes, along with their cellular roles, need to be established as objective biomarkers in conjunction with various biological signals, such as walking speed, brain waves, and clinical data. The biological age/aging clock, determined by methylated DNA, has attracted attention, and calorie restriction not only slows the progression of aging, but also seems to suppress it. However, as indicated by gene expression analysis in aging mice, aging is not a linear model, but is represented by nonlinear dynamic changes. Consequently, the development of experimental models and analytical methods that enhance temporal resolution through time-series analysis, tailored to spatial resolution, such as cell distribution and organ specificity, is progressing. Moreover, in recent years, in addition to anti-aging efforts targeting epigenomic variations, global attention has increasingly focused on research and development aimed at rejuvenating treatments, thus leading to the birth of many biotech companies. Aging Hallmarks such as inflammation, stem cells, metabolism, genomic instability, and autophagy, interact closely with the epigenome. Various postnatal and reversible epigenomic controls of aging, including Yamanaka factors (OKSM and OSK), are now entering a new phase. In the future, the development of aging control using diverse modalities, such as mRNA, artificial peptides, and genome editing, is expected, along with an improved molecular understanding of aging and identification of useful biomarkers.
表观基因组可以充分调控基因的开关状态,以应对外部环境因素和压力。近年来,人们观察到,通过 DNA 甲基化、组蛋白修饰和染色质重塑调节的表观基因组会随着年龄的增长而发生变化。表观基因组的改变会导致细胞特异性表观基因组/特性的丧失,进而引发组织功能的衰退。在哺乳动物中,出生后表观基因组的变化不仅由糖尿病或DNA损伤等代谢性疾病引起,也由社会压力和传染病引起。与全基因组关联研究(GWAS)不同,动态变化的表观基因组及其细胞作用需要与步行速度、脑电波和临床数据等各种生物信号结合起来,作为客观的生物标志物。由甲基化 DNA 决定的生物年龄/衰老时钟已引起人们的关注,卡路里限制不仅能减缓衰老进程,似乎还能抑制衰老。然而,衰老小鼠的基因表达分析表明,衰老不是一个线性模型,而是表现为非线性的动态变化。因此,通过时间序列分析提高时间分辨率的实验模型和分析方法,以及针对细胞分布和器官特异性等空间分辨率的实验模型和分析方法的开发正在取得进展。此外,近年来,除了以表观基因组变异为目标的抗衰老工作外,全球的注意力也越来越多地集中在旨在恢复青春活力的治疗方法的研发上,从而催生了许多生物技术公司。炎症、干细胞、新陈代谢、基因组不稳定性和自噬等衰老标志与表观基因组密切相关。目前,包括山中因子(OKSM 和 OSK)在内的各种产后可逆表观基因组控制衰老的研究正进入一个新阶段。未来,随着对衰老的分子认识和有用生物标志物的确定,利用 mRNA、人工肽和基因组编辑等多种方式控制衰老的研究有望得到发展。
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