eLife (Dec 2020)

Translation in amino-acid-poor environments is limited by tRNAGln charging

  • Natalya N Pavlova,
  • Bryan King,
  • Rachel H Josselsohn,
  • Sara Violante,
  • Victoria L Macera,
  • Santosha A Vardhana,
  • Justin R Cross,
  • Craig B Thompson

DOI
https://doi.org/10.7554/eLife.62307
Journal volume & issue
Vol. 9

Abstract

Read online

An inadequate supply of amino acids leads to accumulation of uncharged tRNAs, which can bind and activate GCN2 kinase to reduce translation. Here, we show that glutamine-specific tRNAs selectively become uncharged when extracellular amino acid availability is compromised. In contrast, all other tRNAs retain charging of their cognate amino acids in a manner that is dependent upon intact lysosomal function. In addition to GCN2 activation and reduced total translation, the reduced charging of tRNAGln in amino-acid-deprived cells also leads to specific depletion of proteins containing polyglutamine tracts including core-binding factor α1, mediator subunit 12, transcriptional coactivator CBP and TATA-box binding protein. Treating amino-acid-deprived cells with exogenous glutamine or glutaminase inhibitors restores tRNAGln charging and the levels of polyglutamine-containing proteins. Together, these results demonstrate that the activation of GCN2 and the translation of polyglutamine-encoding transcripts serve as key sensors of glutamine availability in mammalian cells.

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