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线粒体DNA对人类寿命的影响:来自百岁老人研究的视角。

The impact of mitochondrial DNA on human lifespan: a view from studies on centenarians.

作者信息

Salvioli Stefano, Capri Miriam, Santoro Aurelia, Raule Nicola, Sevini Federica, Lukas Stella, Lanzarini Catia, Monti Daniela, Passarino Giuseppe, Rose Giuseppina, De Benedictis Giovanna, Franceschi Claudio

机构信息

Department of Experimental Pathology, University of Bologna, Bologna, Italy.

出版信息

Biotechnol J. 2008 Jun;3(6):740-9. doi: 10.1002/biot.200800046.

Abstract

The role of inherited and somatic mutations of mitochondrial DNA (mtDNA) in aging and longevity is complex and highly controversial, owing to its peculiar genetics, including the phenomenon of heteroplasmy. Most of the data on mtDNA and longevity have been obtained on humans and particularly on centenarians, i. e., people who escaped or delayed the major age-related pathologies and reached the extreme limit of human lifespan. In this review we summarize the most recent advances in this field that suggest a consistent role in human longevity of both germ-line inherited and somatically acquired mutations. The particular case of the association with longevity of the somatic C150T mutation is extensively discussed, challenging the tenet that mtDNA mutations are basically detrimental. We also stress several limitations of our present knowledge, regarding the difficulty in extrapolating to humans the results obtained in animal models, owing to a variety of biological differences, including the very limited genetic variability of mtDNA in the strains used in laboratory experiments. The use of high-throughput technologies and the extensive analysis, possibly at the single cell level, of different tissues and cell types derived from the same individual will help in disentangling the complexity of mtDNA in aging and longevity.

摘要

线粒体DNA(mtDNA)的遗传突变和体细胞突变在衰老和长寿中的作用复杂且极具争议,这归因于其独特的遗传学特性,包括异质性现象。大多数关于mtDNA与长寿的数据来自人类,尤其是百岁老人,即那些逃脱或延缓了主要年龄相关疾病并达到人类寿命极限的人。在这篇综述中,我们总结了该领域的最新进展,这些进展表明种系遗传突变和体细胞获得性突变在人类长寿中都发挥着一致的作用。我们广泛讨论了体细胞C150T突变与长寿关联的特殊情况,对mtDNA突变基本上有害这一观点提出了挑战。我们还强调了目前知识的几个局限性,由于包括实验室实验所用菌株中mtDNA的遗传变异性非常有限在内的各种生物学差异,难以将在动物模型中获得的结果外推至人类。使用高通量技术以及对来自同一个体的不同组织和细胞类型进行广泛分析(可能在单细胞水平),将有助于厘清mtDNA在衰老和长寿中的复杂性。

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