Role of mitochondrial DNA in longevity, aging and age-related diseases in humans: a reappraisal.

The Italian journal of biochemistry Pub Date : 2007-12-01
Federica Sevini, Aurelia Santoro, Nicola Raule, Francesco Lescai, Claudio Franceschi
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Abstract

The genetic variability of H. sapiens mitochondrial DNA (mtDNA) can be either germ-line inherited or somatically acquired, and its effect on aging and longevity as well as on the pathogenesis of complex age-related diseases is a hot topic. Here we illustrate the complexity of such studies, related to the large genetic variability of mtDNA in different populations and the fact that the rate of the aging process is different in different cells, tissues and organs. As far as concern Alzheimer's disease, the accumulation of somatic mutations in several tissues have been investigated, as well as the inherited mtDNA variability. However, the issue is still controversial and further studies are needed to clarify the role of mtDNA variants in Alzheimer's disease. This review is aimed to summarize the most recent advances in this field. By high throughput mtDNA sequencing and the study of large cohorts of ethnically homogeneous subjects/patients, it is now possible to perform high dimensionality studies in order to clarify the genetic associations among several inherited mtDNA variants and longevity or age-associated diseases in humans.

线粒体DNA在人类寿命、衰老和年龄相关疾病中的作用:重新评估。
智人线粒体DNA (mtDNA)的遗传变异既可以是种系遗传的,也可以是体细胞获得的,其对衰老和长寿以及复杂年龄相关疾病发病机制的影响一直是人们关注的热点。在这里,我们说明了这类研究的复杂性,这与不同人群中mtDNA的巨大遗传变异性以及不同细胞、组织和器官中衰老过程的速度不同有关。就阿尔茨海默病而言,已经研究了几种组织中体细胞突变的积累,以及遗传的mtDNA变异性。然而,这个问题仍然存在争议,需要进一步的研究来阐明mtDNA变异在阿尔茨海默病中的作用。本文综述了这一领域的最新进展。通过高通量mtDNA测序和对种族同质受试者/患者的大队列研究,现在可以进行高维度研究,以澄清几种遗传mtDNA变异与人类长寿或年龄相关疾病之间的遗传关联。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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