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Insights into the mechanisms of eukaryotic translation gained with ribosome profiling

机译:用核糖体分析获得真核翻译机制的见解

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摘要

The development of Ribosome Profiling (RiboSeq) has revolutionized functional genomics. RiboSeq is based on capturing and sequencing of the mRNA fragments enclosed within the translating ribosome and it thereby provides a ` snapshot' of ribosome positions at the transcriptome wide level. Although the method is predominantly used for analysis of differential gene expression and discovery of novel translated ORFs, the RiboSeq data can also be a rich source of information about molecular mechanisms of polypeptide synthesis and translational control. This review will focus on how recent findings made with RiboSeq have revealed important details of the molecular mechanisms of translation in eukaryotes. These include mRNA translation sensitivity to drugs affecting translation initiation and elongation, the roles of upstream ORFs in response to stress, the dynamics of elongation and termination as well as details of intrinsic ribosome behavior on the mRNA after translation termination. As the RiboSeq method is still at a relatively early stage we will also discuss the implications of RiboSeq artifacts on data interpretation.
机译:核糖体分析(Riboseq)的发展具有彻底的功能基因组学。 Riboseq基于捕获和测序封闭在平移核糖体内的mRNA片段,从而在转录组宽水平下提供核糖体位置的“快照”。虽然该方法主要用于分析差异基因的表达和新型翻译ORF的发现,但是Riboseq数据也可以是有关多肽合成和平移控制的分子机制的丰富信息来源。本综述将侧重于利用riboseq最近发现的发现揭示了真核生物中翻译的分子机制的重要细节。这些包括对影响翻译引发和伸长的药物的mRNA平移敏感性,上游ORF响应应力的作用,伸长率和终端的动态以及翻译终止后mRNA上的内在核糖体行为的细节。随着Riboseq方法仍处于相对较早的阶段,我们还将讨论Riboseq伪影对数据解释的影响。

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