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Mitochondrial Aging and Physical Decline: Insights From Three Generations of Women

机译:线粒体衰老与身体衰退:三代女性的见解

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摘要

Decline in mitochondrial DNA (mtDNA) copy number, function, and accumulation of mutations and deletions have been proposed to contribute to age-related physical decline, based on cross sectional studies in genetically unrelated individuals. There is wide variability of mtDNA and functional measurements in many population studies and therefore we assessed mitochondrial function and physical function in 18 families of grandmothers, mothers, and daughters who share the same maternally inherited mtDNA sequence. A significant age-related decline in mtDNA copy number, mitochondrial protein expression, citrate synthase activity, cytochrome c oxidase content, and VO2 peak were observed. Also, a lower abundance of SIRT3, accompanied by an increase in acetylated skeletal muscle proteins, was observed in grandmothers. Muscle tissue–based full sequencing of mtDNA showed greater than 5% change in minor allele frequency over a lifetime in two locations, position 189 and 408 in the noncoding D-loop region but no changes were noted in blood cells mtDNA. The decline in oxidative capacity and muscle function with age in three generations of women who share the same mtDNA sequence are associated with a decline in muscle mtDNA copy number and reduced protein deacetylase activity of SIRT3.
机译:根据与遗传无关的个体的横断面研究,线粒体DNA(mtDNA)的拷贝数,功能以及突变和缺失的积累下降已被认为有助于与年龄相关的身体衰退。在许多人群研究中,mtDNA和功能测量存在很大差异,因此,我们评估了18个共享相同母体遗传mtDNA序列的祖母,母亲和女儿的线粒体功能和身体功能。观察到与年龄相关的mtDNA拷贝数,线粒体蛋白表达,柠檬酸合酶活性,细胞色素c氧化酶含量和VO2峰的显着下降。同样,在祖母中观察到较低的SIRT3丰度,并伴有乙酰化的骨骼肌蛋白增加。基于肌肉组织的mtDNA完整测序显示,在整个生命周期中,两个等位基因(在非编码D环区域中的位置189和408)的次要等位基因频率变化大于5%,但在血细胞mtDNA中未发现任何变化。在具有相同mtDNA序列的三代女性中,氧化能力和肌肉功能随着年龄的增长而下降,与肌肉mtDNA拷贝数下降和SIRT3蛋白质脱乙酰酶活性降低有关。

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