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自愿轮跑对衰老的 PolG 小鼠模型的大脑和肝脏线粒体 DNA 拷贝数或突变测量没有影响。

Voluntary wheel running has no impact on brain and liver mitochondrial DNA copy number or mutation measures in the PolG mouse model of aging.

机构信息

Beckman Institute, University of Illinois at Urbana-Champaign, Urbana, Illinois, United States of America.

Neuroscience Program, Beckman Institute, University of Illinois at Urbana-Champaign, Urbana, Illinois, United States of America.

出版信息

PLoS One. 2020 Mar 2;15(3):e0226860. doi: 10.1371/journal.pone.0226860. eCollection 2020.

Abstract

The mitochondrial theory of aging attributes much of the aging process to mitochondrial DNA damage. The polymerase gamma (PolG) mutant mouse was designed to evaluate this theory and thus carries a mutated proofreading region of polymerase gamma (D257A) that exclusively transcribes the mitochondrial genome. As a result, PolGD257A mice accumulate mitochondrial DNA (mtDNA) mutations that lead to premature aging, as evidenced by hair loss, weight loss, kyphosis, increased rates of apoptosis, organ damage, and an early death, occurring around 12 months of age. Research has shown that exercise decreases skeletal muscle mtDNA mutations and normalizes protein levels in PolG mice. However, brain mtDNA changes with exercise in PolG mice have not been studied. We found no effects of exercise on mtDNA mutations or copy number in either the brain or liver of PolG mice, despite changes to body mass. Our results suggest that mitochondrial mutations play little role in exercise-brain interactions in the PolG model of accelerated aging. In addition to evaluating the effect of exercise on mtDNA outcomes, we also implemented novel methods for both extracting mtDNA and measuring mtDNA mutations, with aims for improving the efficiency and accuracy of these methods.

摘要

衰老的线粒体理论将衰老过程的很大一部分归因于线粒体 DNA 损伤。聚合酶γ(PolG)突变鼠被设计用来评估这一理论,因此携带一个突变的聚合酶γ(D257A)校对区域,该区域专门转录线粒体基因组。结果,PolGD257A 小鼠积累线粒体 DNA(mtDNA)突变,导致过早衰老,表现为脱发、体重减轻、脊柱后凸、细胞凋亡率增加、器官损伤和 12 个月左右的早逝。研究表明,运动可减少骨骼肌 mtDNA 突变并使 PolG 小鼠中的蛋白质水平正常化。然而,运动对 PolG 小鼠大脑中线粒体 DNA 的变化尚未研究。尽管体重发生了变化,但我们发现运动对 PolG 小鼠大脑或肝脏中的 mtDNA 突变或拷贝数没有影响。我们的结果表明,线粒体突变在加速衰老的 PolG 模型中,在运动与大脑的相互作用中作用不大。除了评估运动对 mtDNA 结果的影响外,我们还实施了新的 mtDNA 提取和 mtDNA 突变测量方法,旨在提高这些方法的效率和准确性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eb96/7051064/f98e8f3c4557/pone.0226860.g001.jpg

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