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线粒体基因组动态中的偶然性与选择。

Contingency and selection in mitochondrial genome dynamics.

机构信息

Department of Physics, University of Toronto, Toronto, Canada.

IBBME, University of Toronto, Toronto, Canada.

出版信息

Elife. 2022 Apr 11;11:e76557. doi: 10.7554/eLife.76557.

Abstract

High frequencies of mutant mitochondrial DNA (mtDNA) in human cells lead to cellular defects that are associated with aging and disease. Yet much remains to be understood about the dynamics of the generation of mutant mtDNAs and their relative replicative fitness that informs their fate within cells and tissues. To address this, we utilize long-read single-molecule sequencing to track mutational trajectories of mtDNA in the model organism . This model has numerous advantages over mammalian systems due to its much larger mtDNA and ease of artificially competing mutant and wild-type mtDNA copies in cells. We show a previously unseen pattern that constrains subsequent excision events in mtDNA fragmentation in yeast. We also provide evidence for the generation of rare and contentious non-periodic mtDNA structures that lead to persistent diversity within individual cells. Finally, we show that measurements of relative fitness of mtDNA fit a phenomenological model that highlights important biophysical parameters governing mtDNA fitness. Altogether, our study provides techniques and insights into the dynamics of large structural changes in genomes that we show are applicable to more complex organisms like humans.

摘要

人类细胞中高频的突变线粒体 DNA(mtDNA)会导致与衰老和疾病相关的细胞缺陷。然而,对于突变 mtDNA 的产生及其相对复制适应性的动态,以及它们在细胞和组织内的命运,我们仍有许多需要了解。为了解决这个问题,我们利用长读长单分子测序技术来追踪模型生物中的 mtDNA 突变轨迹。与哺乳动物系统相比,该模型具有许多优势,因为它的 mtDNA 更大,并且更容易在细胞中人为竞争突变型和野生型 mtDNA 拷贝。我们展示了一种以前未见的模式,这种模式限制了酵母 mtDNA 片段化中随后的切除事件。我们还提供了证据,证明了稀有和有争议的非周期性 mtDNA 结构的产生,这些结构导致了单个细胞内的持续多样性。最后,我们表明,mtDNA 相对适应性的测量符合一个现象学模型,该模型突出了控制 mtDNA 适应性的重要生物物理参数。总之,我们的研究提供了技术和对基因组中大型结构变化的动态的深入了解,我们表明这些变化适用于更复杂的生物体,如人类。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5fcf/9054137/43b4890bc93b/elife-76557-fig1.jpg

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