Peptidyl tRNA hydrolase is required for robust prolyl-tRNA turnover inMycobacterium tuberculosis

Author:

Tomasi Francesca G.ORCID,Schweber Jessica T. P.,Kimura SatoshiORCID,Zhu JunhaoORCID,Cleghorn Laura A. T.,Davis Susan H.,Green Simon R.,Waldor Matthew K.ORCID,Rubin Eric J.

Abstract

AbstractEnzymes involved in rescuing stalled ribosomes and recycling translation machinery are ubiquitous in bacteria and required for growth. Peptidyl tRNA drop-off is a type of abortive translation that results in the release of a truncated peptide that is still bound to tRNA (peptidyl tRNA) into the cytoplasm. Peptidyl tRNA hydrolase (Pth) recycles the released tRNA by cleaving off the unfinished peptide and is essential in most bacterial species. We developed a sequencing-based strategy called Cu-tRNAseq to study the physiological role of Pth inMycobacterium tuberculosis(Mtb). While most peptidyl tRNA species accumulated in a strain with impaired Pth expression, peptidyl prolyl-tRNA was particularly enriched, suggesting that Pth is required for robust peptidyl prolyl-tRNA turnover. Reducing Pth levels increasedMtb’s susceptibility to tRNA synthetase inhibitors that are in development to treat tuberculosis (TB) and rendered this pathogen highly susceptible to macrolides, drugs that are ordinarily ineffective againstMtb. Collectively, our findings reveal the potency of Cu-tRNAseq for profiling peptidyl tRNAs and suggest that targeting Pth would open new therapeutic approaches for TB.

Publisher

Cold Spring Harbor Laboratory

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