Gain of C-Ala enables AlaRS to target the L-shaped tRNAAla

Author:

Antika Titi Rindi1,Chrestella Dea Jolie1,Ivanesthi Indira Rizqita1,Rida Gita Riswana Nawung1,Chen Kuan-Yu1,Liu Fu-Guo1,Lee Yi-Chung2,Chen Yu-Wei3,Tseng Yi-Kuan4,Wang Chien-Chia1ORCID

Affiliation:

1. Department of Life Sciences, National Central University, Zhongli District, Taoyuan 32001, Taiwan

2. Department of Neurology, Taipei Veterans General Hospital, Beitou District, Taipei 11217, Taiwan

3. Department of Neurology, Landseed International Hospital, Pingzhen District, Taoyuan 32449, Taiwan

4. Graduate Institute of Statistics, National Central University, Zhongli District, Taoyuan 32001, Taiwan

Abstract

Abstract Unlike many other aminoacyl-tRNA synthetases, alanyl-tRNA synthetase (AlaRS) retains a conserved prototype structure throughout biology. While Caenorhabditis elegans cytoplasmic AlaRS (CeAlaRSc) retains the prototype structure, its mitochondrial counterpart (CeAlaRSm) contains only a residual C-terminal domain (C-Ala). We demonstrated herein that the C-Ala domain from CeAlaRSc robustly binds both tRNA and DNA. It bound different tRNAs but preferred tRNAAla. Deletion of this domain from CeAlaRSc sharply reduced its aminoacylation activity, while fusion of this domain to CeAlaRSm selectively and distinctly enhanced its aminoacylation activity toward the elbow-containing (or L-shaped) tRNAAla. Phylogenetic analysis showed that CeAlaRSm once possessed the C-Ala domain but later lost most of it during evolution, perhaps in response to the deletion of the T-arm (part of the elbow) from its cognate tRNA. This study underscores the evolutionary gain of C-Ala for docking AlaRS to the L-shaped tRNAAla.

Funder

Ministry of Science and Technology, Taiwan

Landseed Hospital

Taipei Veterans General Hospital

University System of Taiwan

Publisher

Oxford University Press (OUP)

Subject

Genetics

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