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线粒体与核基因组学和衰老。

Mitonuclear genomics and aging.

机构信息

Leonard Davis School of Gerontology, University of Southern California, Los Angeles, CA, 90089, USA.

USC Norris Comprehensive Cancer Center, Los Angeles, CA, 90089, USA.

出版信息

Hum Genet. 2020 Mar;139(3):381-399. doi: 10.1007/s00439-020-02119-5. Epub 2020 Jan 29.

Abstract

Our cells operate based on two distinct genomes that are enclosed in the nucleus and mitochondria. The mitochondrial genome presumably originates from endosymbiotic bacteria. With time, a large portion of the original genes in the bacterial genome is considered to have been lost or transferred to the nuclear genome, leaving a reduced 16.5 Kb circular mitochondrial DNA (mtDNA). Traditionally only 37 genes, including 13 proteins, were thought to be encoded within mtDNA, its genetic repertoire is expanding with the identification of mitochondrial-derived peptides (MDPs). The biology of aging has been largely unveiled to be regulated by genes that are encoded in the nuclear genome, whereas the mitochondrial genome remained more cryptic. However, recent studies position mitochondria and mtDNA as an important counterpart to the nuclear genome, whereby the two organelles constantly regulate each other. Thus, the genomic network that regulates lifespan and/or healthspan is likely constituted by two unique, yet co-evolved, genomes. Here, we will discuss aspects of mitochondrial biology, especially mitochondrial communication that may add substantial momentum to aging research by accounting for both mitonuclear genomes to more comprehensively and inclusively map the genetic and molecular networks that govern aging and age-related diseases.

摘要

我们的细胞基于两个不同的基因组运作,这两个基因组被包含在细胞核和线粒体中。线粒体基因组可能起源于内共生细菌。随着时间的推移,细菌基因组中原来的大部分基因被认为已经丢失或转移到了核基因组中,只剩下一个缩小的 16.5kb 圆形线粒体 DNA(mtDNA)。传统上,只有 37 个基因,包括 13 种蛋白质,被认为是由 mtDNA 编码的,随着线粒体衍生肽(MDPs)的鉴定,其遗传库正在扩大。衰老的生物学在很大程度上被揭示是由核基因组编码的基因调控的,而线粒体基因组仍然更加神秘。然而,最近的研究将线粒体和 mtDNA 定位为核基因组的一个重要对应物,这两个细胞器不断相互调节。因此,调节寿命和/或健康跨度的基因组网络可能由两个独特但共同进化的基因组构成。在这里,我们将讨论线粒体生物学的各个方面,特别是线粒体通讯,它通过考虑到线粒体和核基因组来为衰老研究增添动力,更全面和包容地绘制控制衰老和与年龄相关疾病的遗传和分子网络。

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