Cell Death and Disease (Jul 2024)

The eEF2 kinase coordinates the DNA damage response to cisplatin by supporting p53 activation

  • Jonathan K. M. Lim,
  • Arash Samiei,
  • Alberto Delaidelli,
  • Jessica Oliveira de Santis,
  • Vanessa Brinkmann,
  • Christopher J. Carnie,
  • Daniel Radiloff,
  • Laura Hruby,
  • Alisa Kahler,
  • Jordan Cran,
  • Gabriel Leprivier,
  • Poul H. Sorensen

DOI
https://doi.org/10.1038/s41419-024-06891-4
Journal volume & issue
Vol. 15, no. 7
pp. 1 – 10

Abstract

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Abstract Eukaryotic elongation factor 2 (eEF2) kinase (eEF2K) is a stress-responsive hub that inhibits the translation elongation factor eEF2, and consequently mRNA translation elongation, in response to hypoxia and nutrient deprivation. EEF2K is also involved in the response to DNA damage but its role in response to DNA crosslinks, as induced by cisplatin, is not known. Here we found that eEF2K is critical to mediate the cellular response to cisplatin. We uncovered that eEF2K deficient cells are more resistant to cisplatin treatment. Mechanistically, eEF2K deficiency blunts the activation of the DNA damage response associated ATM and ATR pathways, in turn preventing p53 activation and therefore compromising induction of cisplatin-induced apoptosis. We also report that loss of eEF2K delays the resolution of DNA damage triggered by cisplatin, suggesting that eEF2K contributes to DNA damage repair in response to cisplatin. In support of this, our data shows that eEF2K promotes the expression of the DNA repair protein ERCC1, critical for the repair of cisplatin-caused DNA damage. Finally, using Caenorhabditis elegans as an in vivo model, we find that deletion of efk-1, the worm eEF2K ortholog, mitigates the induction of germ cell death in response to cisplatin. Together, our data highlight that eEF2K represents an evolutionary conserved mediator of the DNA damage response to cisplatin which promotes p53 activation to induce cell death, or alternatively facilitates DNA repair, depending on the extent of DNA damage.