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人类线粒体前体tRNASer(UCN)中的自然发生突变会影响转移核糖核酸酶Z的切割位点、加工动力学和底物二级结构。

Naturally occurring mutations in human mitochondrial pre-tRNASer(UCN) can affect the transfer ribonuclease Z cleavage site, processing kinetics, and substrate secondary structure.

作者信息

Yan Hua, Zareen Neela, Levinger Louis

机构信息

York College of The City University of New York, Jamaica, 11451, USA.

出版信息

J Biol Chem. 2006 Feb 17;281(7):3926-35. doi: 10.1074/jbc.M509822200. Epub 2005 Dec 16.

Abstract

tRNAs are transcribed as precursors with a 5' end leader and a 3' end trailer. The 5' end leader is processed by RNase P, and in most organisms in all three kingdoms, transfer ribonuclease (tRNase) Z can endonucleolytically remove the 3' end trailer. Long ((L)) and short ((S)) forms of the tRNase Z gene are present in the human genome. tRNase Z(L) processes a nuclear-encoded pre-tRNA approximately 1600-fold more efficiently than tRNase Z(S) and is predicted to have a strong mitochondrial transport signal. tRNase Z(L) could, thus, process both nuclear- and mitochondrially encoded pre-tRNAs. More than 150 pathogenesis-associated mutations have been found in the mitochondrial genome, most of them in the 22 mitochondrially encoded tRNAs. All the mutations investigated in human mitochondrial tRNA(Ser(UCN)) affect processing efficiency, and some affect the cleavage site and secondary structure. These changes could affect tRNase Z processing of mutant pre-tRNAs, perhaps contributing to mitochondrial disease.

摘要

转运RNA(tRNA)最初转录生成的前体带有5'端前导序列和3'端拖尾序列。5'端前导序列由核糖核酸酶P进行加工处理,并且在所有三个生物界的大多数生物体中,转移核糖核酸酶(tRNase)Z能够通过内切核酸酶作用去除3'端拖尾序列。人类基因组中存在tRNase Z基因的长(L)和短(S)两种形式。tRNase Z(L)对核编码的前体tRNA的加工效率比tRNase Z(S)高出约1600倍,并且预计具有很强的线粒体转运信号。因此,tRNase Z(L)可以加工核编码和线粒体编码的前体tRNA。在线粒体基因组中已经发现了150多个与发病机制相关的突变,其中大多数位于22个线粒体编码的tRNA中。在人类线粒体tRNA(Ser(UCN))中研究的所有突变都会影响加工效率,有些还会影响切割位点和二级结构。这些变化可能会影响突变前体tRNA的tRNase Z加工过程,这或许是导致线粒体疾病的原因之一。

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