Aging-associated accumulation of mitochondrial DNA mutations in tumor origin

Aging-associated accumulation of mitochondrial DNA mutations in tumor origin

The majority of cancer patients are among aged population, suggesting an urgent need to advance our knowledge on complicated relationship between aging and cancer. It has been hypothesized that metabolic changes during aging could act as a driver for tumorigenesis. Given the fact that mitochondrial...

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Veröffentlicht in:Life medicine 2022-10, Vol.1 (2), p.149-167
Hauptverfasser: Kong, Minghua, Guo, Lishu, Xu, Weilin, He, Chengpeng, Jia, Xiaoyan, Zhao, Zhiyao, Gu, Zhenglong
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container_end_page 167
container_issue 2
container_start_page 149
container_title Life medicine
container_volume 1
creator Kong, Minghua
Guo, Lishu
Xu, Weilin
He, Chengpeng
Jia, Xiaoyan
Zhao, Zhiyao
Gu, Zhenglong
description The majority of cancer patients are among aged population, suggesting an urgent need to advance our knowledge on complicated relationship between aging and cancer. It has been hypothesized that metabolic changes during aging could act as a driver for tumorigenesis. Given the fact that mitochondrial DNA (mtDNA) mutations are common in both tumors and aged tissues, it is interesting to contemplate possible role of age-related mtDNA mutations in tumorigenesis. MtDNA encodes genes essential for mitochondrial metabolism, and mtDNA mutates at a much higher rate than nuclear genome. Random drifting of somatic mtDNA mutations, as a result of cell division or mitochondrial turnover during aging, may lead to more and more cells harboring high-frequency pathogenic mtDNA mutations, albeit at different loci, in single-cells. Such mutations can induce metabolic reprogramming, nuclear genome instability and immune response, which might increase the likelihood of tumorigenesis. In this review, we summarize current understanding of how mtDNA mutations accumulate with aging and how these mutations could mechanistically contribute to tumor origin. We also discuss potential prevention strategies for mtDNA mutation-induced tumorigenesis, and future works needed in this direction.
doi_str_mv 10.1093/lifemedi/lnac014
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title Aging-associated accumulation of mitochondrial DNA mutations in tumor origin
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