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呼吸缺陷型酵母线粒体tRNA突变体的氨酰化作用和构象特性

Aminoacylation and conformational properties of yeast mitochondrial tRNA mutants with respiratory deficiency.

作者信息

Francisci Silvia, DE Luca Cristina, Oliva Romina, Morea Veronica, Tramontano Anna, Frontali Laura

机构信息

Department of Cell and Developmental Biology, University of Rome La Sapienza, Italy.

出版信息

RNA. 2005 Jun;11(6):914-27. doi: 10.1261/rna.2260305.

Abstract

We report the identification and characterization of eight yeast mitochondrial tRNA mutants, located in mitochondrial tRNA(Gln), tRNA(Arg2), tRNA(Ile), tRNA(His), and tRNA(Cys), the respiratory phenotypes of which exhibit various degrees of deficiency. The mutations consist in single-base substitutions, insertions, or deletions, and are distributed all over the tRNA sequence and structure. To identify the features responsible for the defective phenotypes, we analyzed the effect of the different mutations on the electrophoretic mobility and efficiency of acylation of the mutated tRNAs in comparison with the respective wild-type molecules. Five of the studied mutations determine both conformational changes and defective acylation, while two have neither or limited effect. However, variations in structure and acylation are not necessarily correlated; the remaining mutation affects the tRNA conformation, but not its acylation properties. Analysis of tRNA structures and of mitochondrial and cytoplasmic yeast tRNA sequences allowed us to propose explanations for the observed defects, which can be ascribed to either the loss of identity nucleotides or, more often, of specific secondary and/or tertiary interactions that are largely conserved in native mitochondrial and cytoplasmic tRNAs.

摘要

我们报告了八个酵母线粒体tRNA突变体的鉴定和特征,这些突变体位于线粒体tRNA(Gln)、tRNA(Arg2)、tRNA(Ile)、tRNA(His)和tRNA(Cys)中,其呼吸表型表现出不同程度的缺陷。这些突变包括单碱基替换、插入或缺失,分布在tRNA的整个序列和结构中。为了确定导致缺陷表型的特征,我们分析了与各自野生型分子相比,不同突变对突变tRNA的电泳迁移率和酰化效率的影响。所研究的突变中有五个既导致构象变化又导致酰化缺陷,而另外两个则没有影响或影响有限。然而,结构和酰化的变化不一定相关;其余的突变影响tRNA构象,但不影响其酰化特性。对tRNA结构以及线粒体和细胞质酵母tRNA序列的分析使我们能够对观察到的缺陷提出解释,这些缺陷可归因于识别核苷酸的丧失,或者更常见的是,归因于在天然线粒体和细胞质tRNA中大量保守的特定二级和/或三级相互作用的丧失。

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