eLife (Aug 2021)

Loss of N1-methylation of G37 in tRNA induces ribosome stalling and reprograms gene expression

  • Isao Masuda,
  • Jae-Yeon Hwang,
  • Thomas Christian,
  • Sunita Maharjan,
  • Fuad Mohammad,
  • Howard Gamper,
  • Allen R Buskirk,
  • Ya-Ming Hou

DOI
https://doi.org/10.7554/eLife.70619
Journal volume & issue
Vol. 10

Abstract

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N1-methylation of G37 is required for a subset of tRNAs to maintain the translational reading-frame. While loss of m1G37 increases ribosomal +1 frameshifting, whether it incurs additional translational defects is unknown. Here, we address this question by applying ribosome profiling to gain a genome-wide view of the effects of m1G37 deficiency on protein synthesis. Using E coli as a model, we show that m1G37 deficiency induces ribosome stalling at codons that are normally translated by m1G37-containing tRNAs. Stalling occurs during decoding of affected codons at the ribosomal A site, indicating a distinct mechanism than that of +1 frameshifting, which occurs after the affected codons leave the A site. Enzyme- and cell-based assays show that m1G37 deficiency reduces tRNA aminoacylation and in some cases peptide-bond formation. We observe changes of gene expression in m1G37 deficiency similar to those in the stringent response that is typically induced by deficiency of amino acids. This work demonstrates a previously unrecognized function of m1G37 that emphasizes its role throughout the entire elongation cycle of protein synthesis, providing new insight into its essentiality for bacterial growth and survival.

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