首页> 外文期刊>Nucleic Acids Research >Effect of a mutation in the anticodon of human mitochondrial tRNAPro on its post-transcriptional modification pattern.
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Effect of a mutation in the anticodon of human mitochondrial tRNAPro on its post-transcriptional modification pattern.

机译:人线粒体tRNAPro反密码子中的突变对其转录后修饰模式的影响。

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Although the gene sequences of all 22 tRNAs encoded in the human mitochondrial genome are known, little information exists about their sequences at the RNA level. This becomes a crucial limitation when searching for a molecular understanding of the growing number of maternally inherited human diseases correlated with point mutations in tRNA genes. Here we describe the sequence of human mt-tRNAPropurified from placenta. It shows absence of editing events in this tRNA and highlights the presence of eight post-transcriptional modifications. These include T54, never found so far in an animal mt-tRNA, and m1G37, a modification known to have fundamental functional properties in a number of canonical tRNAs. Occurrence of m1G37 was further investigated in an analysis of the substrate properties of in vitro transcripts of human mt-tRNAProtowards pure Escherichia coli methylguanosine transferase. This enzyme properly methylates G37 in mt-tRNA and is sensitive to the presence of a second G at position 36, neighboring the target nucleotide for methylation. Since mutation of nt 36 was shown to be correlated with myopathy, the potential consequences of non-modification or under-modification of mt-tRNA nucleotides in expression of the particular myopathy and of mitochondrial diseases in general are discussed.
机译:尽管已知人类线粒体基因组中编码的所有22种tRNA的基因序列,但在RNA水平上有关其序列的信息很少。当寻求对与tRNA基因中的点突变相关的越来越多的母亲遗传的人类疾病的分子理解时,这成为关键的局限。在这里,我们描述了从胎盘中纯化的人mt-tRNA的序列。它显示该tRNA中没有编辑事件,并突出显示了八种转录后修饰的存在。其中包括迄今为止尚未在动物mt-tRNA中发现的T54和m1G37(一种在许多典型tRNA中具有基本功能特性的修饰)。在分析人mt-tRNA的体外转录本的底物特性后,进一步研究了m1G37的发生。该酶正确地使mt-tRNA中的G37甲基化,并且对位置36处与甲基化目标核苷酸相邻的第二个G敏感。由于显示出nt 36的突变与肌病有关,因此讨论了在特定肌病和线粒体疾病的表达中,mt-tRNA核苷酸未修饰或修饰不足的潜在后果。

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