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翻译复合物谱测序可区分上游开放阅读框控制的翻译中的渗漏扫描和重新起始。

Translation Complex Profile Sequencing Allows Discrimination of Leaky Scanning and Reinitiation in Upstream Open Reading Frame-controlled Translation.

机构信息

Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry, RAS, 117997 Moscow, Russia; Belozersky Institute of Physico-Chemical Biology, Lomonosov Moscow State University, 119992 Moscow, Russia.

School of Biochemistry and Cell Biology, University College Cork, Cork T12 K8AF, Ireland; SFI Centre for Research Training in Genomics Data Science, University College Cork, Cork T12 K8AF, Ireland.

出版信息

J Mol Biol. 2024 Dec 1;436(23):168850. doi: 10.1016/j.jmb.2024.168850. Epub 2024 Oct 30.

DOI:10.1016/j.jmb.2024.168850
PMID:39486574
Abstract

Upstream open reading frames (uORFs) are a class of translated regions (translons) in mRNA 5' leaders. uORFs are believed to be pervasive regulators of the translation of mammalian mRNAs. Some uORFs are highly repressive but others have little or no impact on downstream mRNA translation either due to inefficient recognition of their start codon(s) or/and due to efficient reinitiation after uORF translation. While experiments with uORF reporter constructs proved to be instrumental in the investigation of uORF-mediated mechanisms of translation control, they can have serious limitations as manipulations with uORF sequences can yield various artefacts. Here we propose a general approach for using translation complex profiling (TCP-seq) data for exploring uORF regulatory characteristics. Using several examples, we show how TCP-seq could be used to estimate both repressiveness and modes of action of individual uORFs. We demonstrate how this approach could be used to assess the mechanisms of uORF-mediated translation control in the mRNA of several human genes, including EIF5, IFRD1, MDM2, MIEF1, PPP1R15B, TAF7, and UCP2.

摘要

上游开放阅读框(uORFs)是 mRNA 5' 先导区中一类翻译区(translons)。uORFs 被认为是哺乳动物 mRNA 翻译的普遍调控因子。一些 uORFs 具有高度抑制性,但由于其起始密码子(s)的识别效率低下,或者由于 uORF 翻译后的有效重新起始,其他 uORFs 对下游 mRNA 翻译几乎没有影响或没有影响。虽然使用 uORF 报告基因构建体的实验被证明对研究 uORF 介导的翻译调控机制非常有帮助,但它们可能存在严重的局限性,因为对 uORF 序列的操作可能会产生各种假象。在这里,我们提出了一种利用翻译复合物分析(TCP-seq)数据来探索 uORF 调控特征的一般方法。我们使用了几个例子,展示了如何使用 TCP-seq 来估计单个 uORF 的抑制性和作用模式。我们展示了如何使用这种方法来评估 uORF 介导的几种人类基因(包括 EIF5、IFRD1、MDM2、MIEF1、PPP1R15B、TAF7 和 UCP2)mRNA 中转录调控的机制。

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