Cell Death and Disease (Nov 2022)

Translational readthrough of nonsense mutant TP53 by mRNA incorporation of 5-Fluorouridine

  • Mireia Palomar-Siles,
  • Angelos Heldin,
  • Meiqiongzi Zhang,
  • Charlotte Strandgren,
  • Viktor Yurevych,
  • Jip T. van Dinter,
  • Sem A. G. Engels,
  • Damon A. Hofman,
  • Susanne Öhlin,
  • Birthe Meineke,
  • Vladimir J. N. Bykov,
  • Sebastiaan van Heesch,
  • Klas G. Wiman

DOI
https://doi.org/10.1038/s41419-022-05431-2
Journal volume & issue
Vol. 13, no. 11
pp. 1 – 17

Abstract

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Abstract TP53 nonsense mutations in cancer produce truncated inactive p53 protein. We show that 5-FU metabolite 5-Fluorouridine (FUr) induces full-length p53 in human tumor cells carrying R213X nonsense mutant TP53. Ribosome profiling visualized translational readthrough at the R213X premature stop codon and demonstrated that FUr-induced readthrough is less permissive for canonical stop codon readthrough compared to aminoglycoside G418. FUr is incorporated into mRNA and can potentially base-pair with guanine, allowing insertion of Arg tRNA at the TP53 R213X UGA premature stop codon and translation of full-length wild-type p53. We confirmed that full-length p53 rescued by FUr triggers tumor cell death by apoptosis. FUr also restored full-length p53 in TP53 R213X mutant human tumor xenografts in vivo. Thus, we demonstrate a novel strategy for therapeutic rescue of nonsense mutant TP53 and suggest that FUr should be explored for treatment of patients with TP53 nonsense mutant tumors.