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Is selection required for the accumulation of somatic mitochondrial DNA mutations in post-mitotic cells?

机译:在有丝分裂后细胞中体细胞线粒体DNA突变的积累是否需要选择?

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摘要

Mitochondrial DNA (mtDNA) mutations accumulate in the skeletal muscle of patients with mtDNA disease, and also as part of healthy ageing. Simulations of human muscle fibres suggest that, over many decades, the continuous destruction and copying of mtDNA (relaxed replication) can lead to dramatic changes in the percentage level of mutant mtDNA in non-dividing cells through random genetic drift. This process should apply to both pathogenic and neutral mutations. To test this hypothesis we sequenced the entire mitochondrial genome for 20 muscle fibres from a healthy elderly 85-year-old individual, chosen because of the low frequency of cytochrome c oxidase negative fibres. Phenotypically neutral single base substitutions were detected in 15% of the healthy fibres, supporting the hypothesis that positive selection is not essential for the clonal expansion of mtDNA point mutations during human life. Treatments that enhance mtDNA replication, such as vigorous excercise, could amplify this process, with potentially detrimental long-term consequences.
机译:线粒体DNA(mtDNA)突变积累在mtDNA疾病患者的骨骼肌中,并且是健康衰老的一部分。人类肌肉纤维的模拟表明,几十年来,mtDNA的连续破坏和复制(松弛复制)可通过随机遗传漂移导致非分裂细胞中突变mtDNA百分比水平的急剧变化。此过程应适用于致病性突变和中性突变。为了验证这一假设,我们对来自健康的85岁老人的20条肌肉纤维的线粒体基因组进行了测序,这是由于细胞色素C氧化酶阴性纤维的频率较低而选择的。从表型上看,在15%的健康纤维中检测到中性单碱基取代,支持以下假设:阳性选择对于人类生活中mtDNA点突变的克隆扩增不是必不可少的。加强mtDNA复制的治疗(例如剧烈运动)可能会放大此过程,并可能造成长期有害的后果。

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