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Human mitochondrial DNA with large deletions repopulates organelles faster than full-length genomes under relaxed copy number control

机译:在宽松的拷贝数控制下,具有较大缺失的人线粒体DNA在细胞器中的繁殖速度比全长基因组更快

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摘要

Partially-deleted mitochondrial DNA (ΔmtDNA) accumulates during aging of postmitotic tissues. This accumulation has been linked to decreased metabolic activity, increased reactive oxygen species formation and the aging process. Taking advantage of cell lines with heteroplasmic mtDNA mutations, we showed that, after severe mtDNA depletion, organelles are quickly and predominantly repopulated with ΔmtDNA, whereas repopulation with the wild-type counterpart is slower. This behavior was not observed for full-length genomes with pathogenic point mutations. The faster repopulation of smaller molecules was supported by metabolic labeling of mtDNA with [~3H] thymidine during relaxed copy number control conditions. We also showed that hybrid cells containing two defective mtDNA haplotypes tend to retain the smaller one as they adjust their normal mtDNA copy number. Taken together, our results indicate that, under relaxed copy number control, ΔmtDNAs repopulate mitochondria more efficiently than full-length genomes.
机译:在有丝分裂后组织的衰老过程中,部分缺失的线粒体DNA(ΔmtDNA)会积累。这种积累与降低的代谢活性,增加的活性氧形成和衰老过程有关。利用具有异质性mtDNA突变的细胞系,我们显示,严重的mtDNA耗尽后,细胞器迅速且主要以ΔmtDNA进行重新填充,而野生型对应物的重新填充则较慢。对于具有致病性点突变的全长基因组,未观察到此行为。在放松的拷贝数控制条件下,用[〜3H]胸苷对mtDNA进行代谢标记,从而支持了较小分子的更快重新繁殖。我们还显示,包含两种缺陷mtDNA单倍型的杂交细胞在调整其正常mtDNA拷贝数时倾向于保留较小的单倍型。两者合计,我们的结果表明,在宽松的拷贝数控制下,ΔmtDNAs比全长基因组更有效地重新组装线粒体。

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