Leucyl-tRNA synthetase editing domain functions as a molecular rheostat to control codon ambiguity in mycoplasma pathogens

Li Li; Andrés Palencia; Tiit Lukk; Zhi Li; Zaida A. Luthey-Schulten; Stephen Cusack; Susan A. Martinis; Michal T. Boniecki

doi:10.1073/pnas.1218374110

Leucyl-tRNA synthetase editing domain functions as a molecular rheostat to control codon ambiguity in mycoplasma pathogens

Li Li, Andrés Palencia, Tiit Lukk, Zhi Li, Zaida A. Luthey-Schulten, Stephen Cusack, Susan A. Martinis, Michal T. Boniecki

Research output: Contribution to journal › Article › peer-review

Abstract

Mycoplasma leucyl-tRNA synthetases (LeuRSs) have been identified in which the connective polypeptide 1 (CP1) amino acid editing domain that clears mischarged tRNAs are missing (Mycoplasmamobile) or highly degenerate (Mycoplasma synoviae). Thus, these enzymes rely on a clearance pathway called pretransfer editing, which hydrolyzesmisactivatedaminoacyl- adenylate intermediate via a nebulous mechanism that has been controversial for decades. Even as the sole fidelity pathway for clearing amino acid selection errors in the pathogenic M. mobile, pretransfer editing is not robust enough to completely block mischarging of tRNALeu, resulting in codon ambiguity and statistical proteins. A high-resolution X-ray crystal structure shows that M. mobile LeuRS structurally overlaps with other LeuRS cores. However, when CP1 domains from different aminoacyl-tRNA synthetases and origins were fused to this common LeuRS core, surprisingly, pretransfer editing was enhanced. It is hypothesized that the CP1 domain evolved as a molecular rheostat to balance multiple functions. These include distal control of specificity and enzyme activity in the ancient canonical core, as well as providing a separate hydrolytic active site for clearing mischarged tRNA.

Original language	English (US)
Pages (from-to)	3817-3822
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	110
Issue number	10
DOIs	https://doi.org/10.1073/pnas.1218374110
State	Published - Mar 5 2013

Keywords

Aminoacylation
Protein evolution
Quality control
Statistical proteins
Translation

ASJC Scopus subject areas

General

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10.1073/pnas.1218374110

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Li, L., Palencia, A., Lukk, T., Li, Z., Luthey-Schulten, Z. A., Cusack, S., Martinis, S. A., & Boniecki, M. T. (2013). Leucyl-tRNA synthetase editing domain functions as a molecular rheostat to control codon ambiguity in mycoplasma pathogens. Proceedings of the National Academy of Sciences of the United States of America, 110(10), 3817-3822. https://doi.org/10.1073/pnas.1218374110

Li, L, Palencia, A, Lukk, T, Li, Z, Luthey-Schulten, ZA, Cusack, S, Martinis, SA & Boniecki, MT 2013, 'Leucyl-tRNA synthetase editing domain functions as a molecular rheostat to control codon ambiguity in mycoplasma pathogens', Proceedings of the National Academy of Sciences of the United States of America, vol. 110, no. 10, pp. 3817-3822. https://doi.org/10.1073/pnas.1218374110

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title = "Leucyl-tRNA synthetase editing domain functions as a molecular rheostat to control codon ambiguity in mycoplasma pathogens",

abstract = "Mycoplasma leucyl-tRNA synthetases (LeuRSs) have been identified in which the connective polypeptide 1 (CP1) amino acid editing domain that clears mischarged tRNAs are missing (Mycoplasmamobile) or highly degenerate (Mycoplasma synoviae). Thus, these enzymes rely on a clearance pathway called pretransfer editing, which hydrolyzesmisactivatedaminoacyl- adenylate intermediate via a nebulous mechanism that has been controversial for decades. Even as the sole fidelity pathway for clearing amino acid selection errors in the pathogenic M. mobile, pretransfer editing is not robust enough to completely block mischarging of tRNALeu, resulting in codon ambiguity and statistical proteins. A high-resolution X-ray crystal structure shows that M. mobile LeuRS structurally overlaps with other LeuRS cores. However, when CP1 domains from different aminoacyl-tRNA synthetases and origins were fused to this common LeuRS core, surprisingly, pretransfer editing was enhanced. It is hypothesized that the CP1 domain evolved as a molecular rheostat to balance multiple functions. These include distal control of specificity and enzyme activity in the ancient canonical core, as well as providing a separate hydrolytic active site for clearing mischarged tRNA.",

keywords = "Aminoacylation, Protein evolution, Quality control, Statistical proteins, Translation",

author = "Li Li and Andr{\'e}s Palencia and Tiit Lukk and Zhi Li and Luthey-Schulten, {Zaida A.} and Stephen Cusack and Martinis, {Susan A.} and Boniecki, {Michal T.}",

note = "Funding Information: The author would like to thank National Basic Research Program of China (2014CB660813), National Key Technology Support Program (2015BAE01B03), National Natural Science Foundation of China (51673148, 51678411, 51373121), Innovation Fund for Technology of China (14C26211200298), Innovation Fund for Technology of Tianjin (14ZXCXGX00776, 14TXGCCX00014), Chang-jiang Scholars and Innovative Research Team in University of Ministry of Education of China (IRT13084) for their financial support.",

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AU - Li, Li

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AU - Li, Zhi

AU - Luthey-Schulten, Zaida A.

AU - Cusack, Stephen

AU - Martinis, Susan A.

AU - Boniecki, Michal T.

N1 - Funding Information: The author would like to thank National Basic Research Program of China (2014CB660813), National Key Technology Support Program (2015BAE01B03), National Natural Science Foundation of China (51673148, 51678411, 51373121), Innovation Fund for Technology of China (14C26211200298), Innovation Fund for Technology of Tianjin (14ZXCXGX00776, 14TXGCCX00014), Chang-jiang Scholars and Innovative Research Team in University of Ministry of Education of China (IRT13084) for their financial support.

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AB - Mycoplasma leucyl-tRNA synthetases (LeuRSs) have been identified in which the connective polypeptide 1 (CP1) amino acid editing domain that clears mischarged tRNAs are missing (Mycoplasmamobile) or highly degenerate (Mycoplasma synoviae). Thus, these enzymes rely on a clearance pathway called pretransfer editing, which hydrolyzesmisactivatedaminoacyl- adenylate intermediate via a nebulous mechanism that has been controversial for decades. Even as the sole fidelity pathway for clearing amino acid selection errors in the pathogenic M. mobile, pretransfer editing is not robust enough to completely block mischarging of tRNALeu, resulting in codon ambiguity and statistical proteins. A high-resolution X-ray crystal structure shows that M. mobile LeuRS structurally overlaps with other LeuRS cores. However, when CP1 domains from different aminoacyl-tRNA synthetases and origins were fused to this common LeuRS core, surprisingly, pretransfer editing was enhanced. It is hypothesized that the CP1 domain evolved as a molecular rheostat to balance multiple functions. These include distal control of specificity and enzyme activity in the ancient canonical core, as well as providing a separate hydrolytic active site for clearing mischarged tRNA.

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Leucyl-tRNA synthetase editing domain functions as a molecular rheostat to control codon ambiguity in mycoplasma pathogens

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