首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Thematic series: tRNAs and aminoacyl-tRNA synthetases in human disease: When a common biological role does not imply common disease outcomes: Disparate pathology linked to human mitochondrial aminoacyl-tRNA synthetases
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Thematic series: tRNAs and aminoacyl-tRNA synthetases in human disease: When a common biological role does not imply common disease outcomes: Disparate pathology linked to human mitochondrial aminoacyl-tRNA synthetases

机译:专题系列:人类疾病中的tRNA和氨酰基-tRNA合成酶:当共同的生物学作用并不意味着常见的疾病结果时:与人类线粒体氨酰基-tRNA合成酶相关的病理学

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摘要

Mitochondrial aminoacyl-tRNA synthetases (mt-aaRSs) are essential components of the mitochondrial translation machinery. The correlation of mitochondrial disorders with mutations in these enzymes has raised the interest of the scientific community over the past several years. Most surprising has been the wide-ranging presentation of clinical manifestations in patients with mt-aaRS mutations, despite the enzymes' common biochemical role. Even among cases where a common physiological system is affected, phenotypes, severity, and age of onset varies depending on which mt-aaRS is mutated. Here, we review work done thus far and propose a categorization of diseases based on tissue specificity that highlights emerging patterns. We further discuss multiple in vitro and in cellulo efforts to characterize the behavior of WT and mutant mt-aaRSs that have shaped hypotheses about the molecular causes of these pathologies. Much remains to do in order to complete our understanding of these proteins. We expect that futher work is likely to result in the discovery of new roles for the mt-aaRSs in addition to their fundamental function in mitochondrial translation, informing the development of treatment strategies and diagnoses.
机译:线粒体氨酰基-tRNA合成酶(mt-aaRSs)是线粒体翻译机制的重要组成部分。在过去的几年中,线粒体疾病与这些酶突变的相关性引起了科学界的兴趣。尽管这些酶具有常见的生化作用,但最令人惊讶的是mt-aaRS突变患者的临床表现范围广泛。即使在影响普通生理系统的情况下,表型,严重性和发病年龄也会根据mt-aaRS突变而有所不同。在这里,我们回顾到目前为止所做的工作,并根据突出显示新模式的组织特异性提出疾病分类。我们进一步讨论了多种体外和细胞内努力,以表征野生型和突变型mt-aaRSs的行为,这些行为塑造了有关这些病理原因的分子假说。为了完成我们对这些蛋白质的理解,还有许多工作要做。我们希望,进一步的工作可能会发现mt-aaRSs在线粒体翻译中的基本功能以及它们的新功能,从而为治疗策略和诊断的发展提供新的作用。

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