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哺乳动物细胞中线粒体 DNA 不稳定性。

Mitochondrial DNA Instability in Mammalian Cells.

机构信息

Department of Medical Biochemistry and Biophysics, Umeå University, Umeå, Sweden.

出版信息

Antioxid Redox Signal. 2022 May;36(13-15):885-905. doi: 10.1089/ars.2021.0091. Epub 2021 Jul 2.

Abstract

The small, multicopy mitochondrial genome (mitochondrial DNA [mtDNA]) is essential for efficient energy production, as alterations in its coding information or a decrease in its copy number disrupt mitochondrial ATP synthesis. However, the mitochondrial replication machinery encounters numerous challenges that may limit its ability to duplicate this important genome and that jeopardize mtDNA stability, including various lesions in the DNA template, topological stress, and an insufficient nucleotide supply. An ever-growing array of DNA repair or maintenance factors are being reported to localize to the mitochondria. We review current knowledge regarding the mitochondrial factors that may contribute to the tolerance or repair of various types of changes in the mitochondrial genome, such as base damage, incorporated ribonucleotides, and strand breaks. We also discuss the newly discovered link between mtDNA instability and activation of the innate immune response. By which mechanisms do mitochondria respond to challenges that threaten mtDNA maintenance? What types of mtDNA damage are repaired, and when are the affected molecules degraded instead? And, finally, which forms of mtDNA instability trigger an immune response, and how? Further work is required to understand the contribution of the DNA repair and damage-tolerance factors present in the mitochondrial compartment, as well as the balance between mtDNA repair and degradation. Finally, efforts to understand the events underlying mtDNA release into the cytosol are warranted. Pursuing these and many related avenues can improve our understanding of what goes wrong in mitochondrial disease. . 36, 885-905.

摘要

线粒体基因组(mtDNA)较小且为多拷贝,对高效能量生成至关重要,因为其编码信息的改变或拷贝数的减少会破坏线粒体 ATP 的合成。然而,线粒体复制机制面临着许多挑战,这些挑战可能限制其复制这个重要基因组的能力并危及 mtDNA 的稳定性,包括 DNA 模板中的各种损伤、拓扑压力和核苷酸供应不足。越来越多的 DNA 修复或维护因子被报道定位于线粒体。我们综述了当前关于可能有助于线粒体容忍或修复线粒体基因组中各种类型变化的线粒体因子的知识,例如碱基损伤、掺入的核苷酸和链断裂。我们还讨论了新发现的 mtDNA 不稳定性与固有免疫反应激活之间的联系。线粒体通过哪些机制应对威胁 mtDNA 维持的挑战?修复哪些类型的 mtDNA 损伤,何时降解受影响的分子?最后,哪种形式的 mtDNA 不稳定性会引发免疫反应,以及如何引发?需要进一步的工作来了解线粒体区室中存在的 DNA 修复和损伤容忍因子的贡献,以及 mtDNA 修复和降解之间的平衡。最后,值得努力理解导致 mtDNA 释放到细胞质中的事件。深入研究这些以及许多相关途径可以提高我们对线粒体疾病中出现问题的理解。. 36, 885-905.

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7b74/9127837/3dff3142fc82/ars.2021.0091_figure1.jpg

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