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真核生物核糖体RNA中snoRNA引导的转录后核苷修饰的合成、功能及异质性

Synthesis, Function, and Heterogeneity of snoRNA-Guided Posttranscriptional Nucleoside Modifications in Eukaryotic Ribosomal RNAs.

作者信息

Henras Anthony K, Plisson-Chastang Célia, Humbert Odile, Romeo Yves, Henry Yves

机构信息

Laboratoire de Biologie Moléculaire Eucaryote, Centre de Biologie Intégrative, Université de Toulouse, CNRS, UPS, Toulouse, France.

Laboratoire de Biologie Moléculaire Eucaryote, Centre de Biologie Intégrative, Université de Toulouse, CNRS, UPS, Toulouse, France.

出版信息

Enzymes. 2017;41:169-213. doi: 10.1016/bs.enz.2017.03.007. Epub 2017 Apr 24.

DOI:10.1016/bs.enz.2017.03.007
PMID:28601222
Abstract

Ribosomal RNAs contain numerous 2'-O-methylated nucleosides and pseudouridines. Methylation of the 2' oxygen of ribose moieties and isomerization of uridines into pseudouridines are catalyzed by C/D and H/ACA small nucleolar ribonucleoprotein particles, respectively. We review the composition, structure, and mode of action of archaeal and eukaryotic C/D and H/ACA particles. Most rRNA modifications cluster in functionally crucial regions of the rRNAs, suggesting they play important roles in translation. Some of these modifications promote global translation efficiency or modulate translation fidelity. Strikingly, recent quantitative nucleoside modification profiling methods have revealed that a subset of modification sites is not always fully modified. The finding of such ribosome heterogeneity is in line with the concept of specialized ribosomes that could preferentially translate specific mRNAs. This emerging concept is supported by findings that some human diseases are caused by defects in the rRNA modification machinery correlated with a significant alteration of IRES-dependent translation.

摘要

核糖体RNA含有众多2'-O-甲基化核苷和假尿苷。核糖部分2'氧的甲基化以及尿苷异构化为假尿苷分别由C/D和H/ACA小核仁核糖核蛋白颗粒催化。我们综述了古细菌和真核生物C/D以及H/ACA颗粒的组成、结构和作用模式。大多数rRNA修饰集中在rRNA的功能关键区域,表明它们在翻译中发挥重要作用。其中一些修饰可提高整体翻译效率或调节翻译保真度。引人注目的是,最近的定量核苷修饰谱分析方法显示,一部分修饰位点并不总是完全被修饰。这种核糖体异质性的发现与专门核糖体的概念相符,专门核糖体可能优先翻译特定的mRNA。一些人类疾病是由rRNA修饰机制缺陷导致的,且与内部核糖体进入位点(IRES)依赖性翻译的显著改变相关,这一发现支持了这一新兴概念。

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