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核帽结合蛋白复合物介导的翻译起始。

Translation initiation mediated by nuclear cap-binding protein complex.

出版信息

BMB Rep. 2017 Apr;50(4):186-193. doi: 10.5483/bmbrep.2017.50.4.007.

Abstract

In mammals, cap-dependent translation of mRNAs is initiated by two distinct mechanisms: cap-binding complex (CBC; a heterodimer of CBP80 and 20)-dependent translation (CT) and eIF4E-dependent translation (ET). Both translation initiation mechanisms share common features in driving cap- dependent translation; nevertheless, they can be distinguished from each other based on their molecular features and biological roles. CT is largely associated with mRNA surveillance such as nonsense-mediated mRNA decay (NMD), whereas ET is predominantly involved in the bulk of protein synthesis. However, several recent studies have demonstrated that CT and ET have similar roles in protein synthesis and mRNA surveillance. In a subset of mRNAs, CT preferentially drives the cap-dependent translation, as ET does, and ET is responsible for mRNA surveillance, as CT does. In this review, we summarize and compare the molecular features of CT and ET with a focus on the emerging roles of CT in translation. [BMB Reports 2017; 50(4): 186-193].

摘要

在哺乳动物中,mRNA 的帽依赖性翻译由两种不同的机制启动:帽结合复合物 (CBC; CBP80 和 20 的异二聚体) 依赖性翻译 (CT) 和 eIF4E 依赖性翻译 (ET)。这两种翻译起始机制在驱动帽依赖性翻译方面具有共同特征;然而,它们可以根据其分子特征和生物学作用彼此区分。CT 主要与 mRNA 监测相关,例如无意义介导的 mRNA 降解 (NMD),而 ET 主要参与大量蛋白质合成。然而,最近的几项研究表明,CT 和 ET 在蛋白质合成和 mRNA 监测中具有相似的作用。在一组 mRNA 中,CT 像 ET 一样优先驱动帽依赖性翻译,而 ET 像 CT 一样负责 mRNA 监测。在这篇综述中,我们总结和比较了 CT 和 ET 的分子特征,重点介绍了 CT 在翻译中的新作用。[BMB 报告 2017;50(4):186-193]。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/35a7/5437962/b45f01ed00d4/bmb-50-186f1.jpg

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