Highly Predictive Reprogramming of tRNA Modifications Is Linked to Selective Expression of Codon-Biased Genes

Chan, Clement T. Y.; Deng, Wenjun; Li, Fugen; DeMott, Michael S.; Babu, I. Ramesh; Begley, Thomas J.; Dedon, Peter C.

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Begley, Thomas J.; Li, Fugen; Chan, Clement T. Y.; Deng, Wenjun; DeMott, Michael S; ... Show more

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Abstract

Cells respond to stress by controlling gene expression at several levels, with little known about the role of translation. Here, we demonstrate a coordinated translational stress response system involving stress-specific reprogramming of tRNA wobble modifications that leads to selective translation of codon-biased mRNAs representing different classes of critical response proteins. In budding yeast exposed to four oxidants and five alkylating agents, tRNA modification patterns accurately distinguished among chemically similar stressors, with 14 modified ribonucleosides forming the basis for a data-driven model that predicts toxicant chemistry with >80% sensitivity and specificity. tRNA modification subpatterns also distinguish S[subscript N]1 from S[subscript N]2 alkylating agents, with S[subscript N]2-induced increases in m[superscript 3]C in tRNA mechanistically linked to selective translation of threonine-rich membrane proteins from genes enriched with ACC and ACT degenerate codons for threonine. These results establish tRNA modifications as predictive biomarkers of exposure and illustrate a novel regulatory mechanism for translational control of cell stress response.

Date issued

2015-03

URI

http://hdl.handle.net/1721.1/106638

Department

Massachusetts Institute of Technology. Center for Environmental Health Sciences; Massachusetts Institute of Technology. Department of Biological Engineering

Journal

Chemical Research in Toxicology

Publisher

American Chemical Society

Citation

Chan, Clement T. Y. et al. “Highly Predictive Reprogramming of tRNA Modifications Is Linked to Selective Expression of Codon-Biased Genes.” Chemical Research in Toxicology 28.5 (2015): 978–988. © 2015 American Chemical Society

Version: Final published version

ISSN

0893-228X

1520-5010

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