Misactivation of multiple starvation responses in yeast by loss of tRNA modifications

Author:

Bruch Alexander1,Laguna Teresa2,Butter Falk2ORCID,Schaffrath Raffael1ORCID,Klassen Roland1ORCID

Affiliation:

1. Institut für Biologie, Fachgebiet Mikrobiologie, Universität Kassel, Heinrich-Plett-Str. 40, 34132 Kassel, Germany

2. Department of Quantitative Proteomics, IMB Mainz, Ackermannweg 4, 55128 Mainz, Germany

Abstract

Abstract Previously, combined loss of different anticodon loop modifications was shown to impair the function of distinct tRNAs in Saccharomyces cerevisiae. Surprisingly, each scenario resulted in shared cellular phenotypes, the basis of which is unclear. Since loss of tRNA modification may evoke transcriptional responses, we characterized global transcription patterns of modification mutants with defects in either tRNAGlnUUG or tRNALysUUU function. We observe that the mutants share inappropriate induction of multiple starvation responses in exponential growth phase, including derepression of glucose and nitrogen catabolite-repressed genes. In addition, autophagy is prematurely and inadequately activated in the mutants. We further demonstrate that improper induction of individual starvation genes as well as the propensity of the tRNA modification mutants to form protein aggregates are diminished upon overexpression of tRNAGlnUUG or tRNALysUUU, the tRNA species that lack the modifications of interest. Hence, our data suggest that global alterations in mRNA translation and proteostasis account for the transcriptional stress signatures that are commonly triggered by loss of anticodon modifications in different tRNAs.

Funder

DFG

Chemical Biology of Native Nucleic Acid Modifications

University of Kassel

Publisher

Oxford University Press (OUP)

Subject

Genetics

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