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从线粒体DNA突变和遗传悖论的视角看衰老。

Aging through the lens of mitochondrial DNA mutations and inheritance paradoxes.

作者信息

Chen Jia, Li Hongyu, Liang Runyu, Huang Yongyin, Tang Qiang

机构信息

Heilongjiang University of Chinese Medicine, Harbin, China.

Second Affiliated Hospital of Heilongjiang University of Chinese Medicine, Harbin, China.

出版信息

Biogerontology. 2024 Dec 27;26(1):33. doi: 10.1007/s10522-024-10175-x.

Abstract

Mitochondrial DNA encodes essential components of the respiratory chain complexes, serving as the foundation of mitochondrial respiratory function. Mutations in mtDNA primarily impair energy metabolism, exerting far-reaching effects on cellular physiology, particularly in the context of aging. The intrinsic vulnerability of mtDNA is increasingly recognized as a key driver in the initiation of aging and the progression of its related diseases. In the field of aging research, it is critical to unravel the intricate mechanisms underpinning mtDNA mutations in living organisms and to elucidate the pathological consequences they trigger. Interestingly, certain effects, such as oxidative stress and apoptosis, may not universally accelerate aging as traditionally perceived. These phenomena demand deeper investigation and a more nuanced reinterpretation of current findings to address persistent scientific uncertainties. By synthesizing recent insights, this review seeks to clarify how pathogenic mtDNA mutations drive cellular senescence and systemic health deterioration, while also exploring the complex dynamics of mtDNA inheritance that may propagate these mutations. Such a comprehensive understanding could ultimately inform the development of innovative therapeutic strategies to counteract mitochondrial dysfunctions associated with aging.

摘要

线粒体DNA编码呼吸链复合物的必需成分,是线粒体呼吸功能的基础。线粒体DNA突变主要损害能量代谢,对细胞生理学产生深远影响,尤其是在衰老的背景下。线粒体DNA的内在脆弱性日益被认为是衰老起始及其相关疾病进展的关键驱动因素。在衰老研究领域,揭示生物体中线粒体DNA突变的复杂机制并阐明它们引发的病理后果至关重要。有趣的是,某些效应,如氧化应激和细胞凋亡,可能并不像传统认为的那样普遍加速衰老。这些现象需要更深入的研究和对当前发现进行更细致入微的重新解释,以解决持续存在的科学不确定性。通过综合近期的见解,本综述旨在阐明致病性线粒体DNA突变如何驱动细胞衰老和全身健康恶化,同时也探讨可能传播这些突变的线粒体DNA遗传的复杂动态。这样全面的理解最终可能为开发创新治疗策略提供依据,以对抗与衰老相关的线粒体功能障碍。

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