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Editing activity for eliminating mischarged tRNAs is essential in mammalian mitochondria

机译:在哺乳动物线粒体中的消除错误的TRNA的编辑活动是必不可少的

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摘要

Accuracy of protein synthesis is enabled by the selection of amino acids for tRNA charging by aminoacyl-tRNA synthetases (ARSs), and further enhanced by the proofreading functions of some of these enzymes for eliminating tRNAs mischarged with noncognate amino acids. Mouse models of editing-defective cytoplasmic alanyl-tRNA synthetase (AlaRS) have previously demonstrated the importance of proofreading for cytoplasmic protein synthesis, with embryonic lethal and progressive neurodegeneration phenotypes. Mammalian mitochondria import their own set of nuclear-encoded ARSs for translating critical polypeptides of the oxidative phosphorylation system, but the importance of editing by the mitochondrial ARSs for mitochondrial proteostasis has not been known. We demonstrate here that the human mitochondrial AlaRS is capable of editing mischarged tRNAs in vitro, and that loss of the proofreading activity causes embryonic lethality in mice. These results indicate that tRNA proofreading is essential in mammalian mitochondria, and cannot be overcome by other quality control mechanisms.
机译:通过选择氨基酸通过氨基酰基-TRNA合成酶(ARS)选择氨基酸的蛋白质合成的准确性,并通过一些这些酶的校样功能进一步增强,用于消除非认知氨基酸的TRNA。术语缺陷细胞质醛族醛醛族醛族醛族合成酶(ALARS)的小鼠模型先前已经证明了校对细胞质蛋白质合成的重要性,具有胚胎致命和渐进神经变性表型。哺乳动物线粒体进口自己的一组核编码的ARS,用于翻译氧化磷酸化系统的关键多肽,但是对线粒体蛋白质的线粒体ARS编辑的重要性尚未知。我们在此证明人体线粒体湖泊能够在体外编辑混蛋TrNA,并且校对活性的损失导致小鼠中的胚胎致死。这些结果表明,TRNA校对在哺乳动物线粒体中必不可少,不能通过其他质量控制机制克服。

著录项

  • 来源
    《Nucleic Acids Research》 |2018年第2期|共12页
  • 作者单位

    Univ Helsinki Res Programs Unit Mol Neurol FIN-00290 Helsinki Finland;

    Chinese Acad Sci State Key Lab Mol Biol CAS Ctr Excellence Mol Cell Sci Shanghai Inst Biochem &

    Cell Biol Shanghai 200031 Peoples R China;

    Univ Helsinki Res Programs Unit Mol Neurol FIN-00290 Helsinki Finland;

    Univ Turku Inst Biomed Turku Ctr Dis Modeling FIN-20520 Turku Finland;

    Univ Helsinki Res Programs Unit Mol Neurol FIN-00290 Helsinki Finland;

    Univ Helsinki Res Programs Unit Mol Neurol FIN-00290 Helsinki Finland;

    Univ Turku Inst Biomed Turku Ctr Dis Modeling FIN-20520 Turku Finland;

    Carleton Coll Dept Chem Northfield MN 55057 USA;

    Chinese Acad Sci State Key Lab Mol Biol CAS Ctr Excellence Mol Cell Sci Shanghai Inst Biochem &

    Cell Biol Shanghai 200031 Peoples R China;

    Univ Helsinki Res Programs Unit Mol Neurol FIN-00290 Helsinki Finland;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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