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Mitochondrial Fusion Is Required for mtDNA Stability in Skeletal Muscle and Tolerance of mtDNA Mutations

机译：线粒体融合是骨骼肌中mtDNA稳定性和mtDNA突变耐受性所必需的

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摘要

Mitochondria are highly mobile and dynamic organelles that continually fuse and divide. These processes allow mitochondria to exchange contents, including mitochondrial DNA (mtDNA). Here we examine the functions of mitochondrial fusion in differentiated skeletal muscle through conditional deletion of the mitofusins Mfn1 and Mfn2, mitochondrial GTPases essential for fusion. Loss of the mitofusins causes severe mitochondrial dysfunction, compensatory mitochondrial proliferation, and muscle atrophy. Mutant mice have severe mtDNA depletion in muscle that precedes physiological abnormalities. Moreover, the mitochondrial genomes of the mutant muscle rapidly accumulate point mutations and deletions. In a related experiment, we find that disruption ofmitochondrial fusion strongly increases mitochondrial dysfunction and lethality in a mouse model with high levels of mtDNA mutations. With its dual function in safeguarding mtDNA integrity and preserving mtDNA function in the face of mutations, mitochondrial fusion is likely to be a protective factor in human disorders associated with mtDNA mutations.

机译：线粒体是高度活动和动态的细胞器，不断融合和分裂。这些过程允许线粒体交换内容物，包括线粒体DNA（mtDNA）。在这里，我们通过有条件地删除线粒体融合蛋白Mfn1和Mfn2（融合必不可少的线粒体GTPases）来研究线粒体融合在分化骨骼肌中的功能。丝裂霉素的损失会导致严重的线粒体功能障碍，代偿性线粒体增殖和肌肉萎缩。突变小鼠的肌肉中存在严重的mtDNA耗尽，而生理异常之前。此外，突变肌肉的线粒体基因组迅速积累点突变和缺失。在一个相关的实验中，我们发现在具有高水平mtDNA突变的小鼠模型中，线粒体融合的破坏会大大增加线粒体功能障碍和致死性。线粒体融合具有双重作用，既可以保护mtDNA完整性，又可以在面对突变时保持mtDNA的功能，因此很可能是与mtDNA突变相关的人类疾病的保护因素。

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《Cell》 |2010年第2期|共10页
作者
Hsiuchen Chen; Marc Vermulst; Yun E. Wang; Anne Chomyn; Tomas A. Prolla; J. Michael McCaffery; David C. Chan;
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原文格式 PDF
正文语种 eng
中图分类细胞生物学;
关键词
Muscle; Stability; Mutations;

机译：肌肉;稳定性;突变;

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专利

1. Mitochondrial Fusion Is Required for mtDNA Stability in Skeletal Muscle and Tolerance of mtDNA Mutations [J] . Hsiuchen Chen, Marc Vermulst, Yun E. Wang, Cell . 2010,第2期

机译：线粒体融合是骨骼肌中mtDNA稳定性和mtDNA突变耐受性所必需的
2. Evidence and age-related distribution of mtDNA D-loop point mutations in skeletal muscle from healthy subjects and mitochondrial patients. [J] . Del Bo R, Bordoni A, Boneschi FM, Journal of the Neurological Sciences: Official Bulletin of the World Federation of Neurology . 2002,第1a2期

机译：健康受试者和线粒体患者骨骼肌中mtDNA D环点突变的证据和年龄相关分布。
3. Context-Dependent Role of Mitochondrial Fusion-Fission in Clonal Expansion of mtDNA Mutations [J] . Zhi Yang Tam, Jan Gruber, Barry Halliwell, PLoS Computational Biology . 2015,第5期

机译：线粒体融合在MTDNA突变的克隆扩增中的线粒体融合的上下文依赖性作用
4. Mitochondrial Genome Instability and mtDNA Depletion in Human Cancers [C] . HSIN-CHEN LEE, PEN-HUI YIN, JIN-CHING LIN, Asian Society for Mitochondrial Research and Medicine . 2005

机译：人类癌症中的线粒体基因组不稳定性和MTDNA枯竭
5. Biochemical and genetic characterization of mitochondrial encephalomyopathies resulting from mitochondrial-DNA (mtDNA) and nuclear DNA (nDNA) mutations. [D] . Zheng, Xianxian. 1990

机译：由线粒体DNA（mtDNA）和核DNA（nDNA）突变引起的线粒体脑肌病的生化和遗传特征。
6. Mitochondrial fusion is required for mtDNA stability in skeletal muscle and tolerance of mtDNA mutations [O] . Hsiuchen Chen, Marc Vermulst, Yun E. Wang, -1

机译：线粒体融合需要骨骼肌和mtDNa突变的线粒体DNa耐受性稳定
7. Mitochondrial Fusion Is Required for mtDNA Stability in Skeletal Muscle and Tolerance of mtDNA Mutations \ud [O] . Chen, Hsiuchen, Vermulst, Marc, Wang, Yun E., 2010

机译：线粒体融合是骨骼肌中mtDNA稳定性和mtDNA突变耐受性的必需\ ud

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