Molecular basis of the multifaceted functions of human leucyl-tRNA synthetase in protein synthesis and beyond

生物 氨基酰基tRNA合成酶 氨酰tRNA合成酶 翻译(生物学) 生物化学 转移RNA 核糖体 蛋白质生物合成 功能(生物学) 机制(生物学) 计算生物学 细胞生物学 核糖核酸 基因 信使核糖核酸 认识论 哲学
作者
Ru-Juan Liu,Tao Long,Hao Li,Jingru Zhao,Jing Li,Mingzhu Wang,Andrés Palencia,Jinzhong Lin,Stephen Cusack,En‐Duo Wang
出处
期刊:Nucleic Acids Research [Oxford University Press]
卷期号:48 (9): 4946-4959 被引量:11
标识
DOI:10.1093/nar/gkaa189
摘要

Abstract Human cytosolic leucyl-tRNA synthetase (hcLRS) is an essential and multifunctional enzyme. Its canonical function is to catalyze the covalent ligation of leucine to tRNALeu, and it may also hydrolyze mischarged tRNAs through an editing mechanism. Together with eight other aminoacyl-tRNA synthetases (AaRSs) and three auxiliary proteins, it forms a large multi-synthetase complex (MSC). Beyond its role in translation, hcLRS has an important moonlight function as a leucine sensor in the rapamycin complex 1 (mTORC1) pathway. Since this pathway is active in cancer development, hcLRS is a potential target for anti-tumor drug development. Moreover, LRS from pathogenic microbes are proven drug targets for developing antibiotics, which however should not inhibit hcLRS. Here we present the crystal structure of hcLRS at a 2.5 Å resolution, the first complete structure of a eukaryotic LRS, and analyze the binding of various compounds that target different sites of hcLRS. We also deduce the assembly mechanism of hcLRS into the MSC through reconstitution of the entire mega complex in vitro. Overall, our study provides the molecular basis for understanding both the multifaceted functions of hcLRS and for drug development targeting these functions.

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