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真核生物翻译起始因子4E结合蛋白:新因子、新定位、新作用

eIF4E-binding proteins: new factors, new locations, new roles.

作者信息

Kamenska Anastasiia, Simpson Clare, Standart Nancy

机构信息

*Department of Biochemistry, University of Cambridge, Cambridge CB2 1QW, U.K.

出版信息

Biochem Soc Trans. 2014 Aug;42(4):1238-45. doi: 10.1042/BST20140063.

Abstract

The cap-binding translation initiation factor eIF4E (eukaryotic initiation factor 4E) is central to protein synthesis in eukaryotes. As an integral component of eIF4F, a complex also containing the large bridging factor eIF4G and eIF4A RNA helicase, eIF4E enables the recruitment of the small ribosomal subunit to the 5' end of mRNAs. The interaction between eIF4E and eIF4G via a YXXXXLϕ motif is regulated by small eIF4E-binding proteins, 4E-BPs, which use the same sequence to competitively bind eIF4E thereby inhibiting cap-dependent translation. Additional eIF4E-binding proteins have been identified in the last 10-15 years, characterized by the YXXXXLϕ motif, and by interactions (many of which remain to be detailed) with RNA-binding proteins, or other factors in complexes that recognize the specific mRNAs. In the present article, we focus on the metazoan 4E-T (4E-transporter)/Cup family of eIF4E-binding proteins, and also discuss very recent examples in yeast, fruitflies and humans, some of which predictably inhibit translation, while others may result in mRNA decay or even enhance translation; altogether considerably expanding our understanding of the roles of eIF4E-binding proteins in gene expression regulation.

摘要

帽结合翻译起始因子eIF4E(真核生物起始因子4E)在真核生物的蛋白质合成中起核心作用。作为eIF4F的一个组成部分,eIF4F是一个还包含大的桥接因子eIF4G和eIF4A RNA解旋酶的复合体,eIF4E能使小核糖体亚基募集到mRNA的5′端。eIF4E与eIF4G通过YXXXXLϕ基序的相互作用受小的eIF4E结合蛋白4E-BPs调控,4E-BPs利用相同序列竞争性结合eIF4E,从而抑制帽依赖性翻译。在过去10至15年中鉴定出了其他eIF4E结合蛋白,其特征在于YXXXXLϕ基序,以及与RNA结合蛋白或识别特定mRNA的复合体中的其他因子的相互作用(其中许多仍有待详细研究)。在本文中,我们重点关注后生动物中eIF4E结合蛋白的4E-T(4E转运蛋白)/Cup家族,还讨论了酵母、果蝇和人类中最近的一些例子,其中一些可预见地抑制翻译,而其他一些可能导致mRNA降解甚至增强翻译;这些例子极大地扩展了我们对eIF4E结合蛋白在基因表达调控中作用的理解。

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