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线粒体 DNA 变体与常见疾病:年龄相关的 mtDNA 突变多样性的数学模型。

Mitochondrial DNA Variants and Common Diseases: A Mathematical Model for the Diversity of Age-Related mtDNA Mutations.

机构信息

Human Aging Research Institute, Nanchang University, Nanchang 330031, China.

Wenzhou Key Laboratory of Birth Defects, Wenzhou Central Hospital, Wenzhou 325000, Zhejiang, China.

出版信息

Cells. 2019 Jun 18;8(6):608. doi: 10.3390/cells8060608.

Abstract

The mitochondrion is the only organelle in the human cell, besides the nucleus, with its own DNA (mtDNA). Since the mitochondrion is critical to the energy metabolism of the eukaryotic cell, it should be unsurprising, then, that a primary driver of cellular aging and related diseases is mtDNA instability over the life of an individual. The mutation rate of mammalian mtDNA is significantly higher than the mutation rate observed for nuclear DNA, due to the poor fidelity of DNA polymerase and the ROS-saturated environment present within the mitochondrion. In this review, we will discuss the current literature showing that mitochondrial dysfunction can contribute to age-related common diseases such as cancer, diabetes, and other commonly occurring diseases. We will then turn our attention to the likely role that mtDNA mutation plays in aging and senescence. Finally, we will use this context to develop a mathematical formula for estimating for the accumulation of somatic mtDNA mutations with age. This resulting model shows that almost 90% of non-proliferating cells would be expected to have at least 100 mutations per cell by the age of 70, and almost no cells would have fewer than 10 mutations, suggesting that mtDNA mutations may contribute significantly to many adult onset diseases.

摘要

线粒体是人类细胞中除细胞核以外唯一具有自身 DNA(mtDNA)的细胞器。由于线粒体对于真核细胞的能量代谢至关重要,因此个体一生中 mtDNA 不稳定是细胞衰老和相关疾病的主要驱动因素,这并不奇怪。由于 DNA 聚合酶保真度差以及线粒体中存在 ROS 饱和环境,哺乳动物 mtDNA 的突变率明显高于核 DNA 的突变率。在这篇综述中,我们将讨论目前的文献,这些文献表明线粒体功能障碍可能导致与年龄相关的常见疾病,如癌症、糖尿病和其他常见疾病。然后,我们将把注意力转向 mtDNA 突变在衰老和衰老中的可能作用。最后,我们将利用这一背景,为估计随年龄增长体细胞 mtDNA 突变的积累建立一个数学公式。该模型表明,到 70 岁时,几乎 90%的非增殖细胞每细胞预计将至少有 100 个突变,几乎没有细胞的突变少于 10 个,这表明 mtDNA 突变可能对许多成年发病疾病有重大贡献。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a711/6627076/e674bc43bd66/cells-08-00608-g001.jpg

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