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衰老的基因组:生命逻辑中一种必要的“恶”。

Aging genomes: a necessary evil in the logic of life.

作者信息

Vijg Jan

机构信息

Department of Genetics, Albert Einstein College of Medicine, New York, NY, USA.

出版信息

Bioessays. 2014 Mar;36(3):282-92. doi: 10.1002/bies.201300127. Epub 2014 Jan 25.

DOI:10.1002/bies.201300127
PMID:24464418
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5985526/
Abstract

Genomes are inherently unstable because of the need for DNA sequence variation as a substrate for evolution through natural selection. However, most multicellular organisms have postmitotic tissues, with limited opportunity for selective removal of cells harboring persistent damage and deleterious mutations, which can therefore contribute to functional decline, disease, and death. Key in this process is the role of genome maintenance, the network of protein products that repair DNA damage and signal DNA damage response pathways. Genome maintenance is beneficial early in life by swiftly eliminating DNA damage or damaged cells, facilitating rapid cell proliferation. However, at later ages accumulation of unrepaired damage and mutations, as well as ongoing cell depletion, promotes cancer, atrophy, and other deleterious effects associated with aging. As such, genome maintenance and its phenotypic sequelae provide yet another example of antagonistic pleiotropy in aging and longevity.

摘要

由于需要DNA序列变异作为通过自然选择进行进化的底物,基因组本质上是不稳定的。然而,大多数多细胞生物具有有丝分裂后组织,选择性清除携带持续性损伤和有害突变的细胞的机会有限,因此这些损伤和突变会导致功能衰退、疾病和死亡。这一过程的关键在于基因组维护的作用,即修复DNA损伤并发出DNA损伤反应信号通路的蛋白质产物网络。基因组维护在生命早期通过迅速消除DNA损伤或受损细胞而具有益处,促进细胞快速增殖。然而,在生命后期,未修复的损伤和突变的积累以及持续的细胞损耗会促进癌症、萎缩以及与衰老相关的其他有害影响。因此,基因组维护及其表型后果为衰老和长寿中的拮抗多效性提供了又一个例子。

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