Metabolism-dependent secondary effect of anti-MAPK cancer therapy on DNA repair-Reference-Cited by-同舟云学术

Metabolism-dependent secondary effect of anti-MAPK cancer therapy on DNA repair

Published:2024-04-08 Issue:2 Volume:6 Page:
ISSN:2632-8674
Container-title:NAR Cancer
language:en
Short-container-title:

Author:

Aubé Fabien¹²,Fontrodona Nicolas¹²,Guiguettaz Laura¹,Vallin Elodie¹,Fabbri Lucilla³⁴⁵,Lapendry Audrey¹²,Vagner Stephan³⁴⁵,Ricci Emiliano P¹,Auboeuf Didier¹²^ORCID

Affiliation:

1. Laboratoire de Biologie et Modélisation de la Cellule, Ecole Normale Supérieure de Lyon, CNRS, UMR 5239, Inserm, U1293, Université Claude Bernard Lyon 1 , 46 allée d’Italie F-69364 Lyon , France

2. Equipe Labellisée Ligue Nationale Contre le Cancer , LBMC, ENS, Lyon , France

3. Institut Curie, PSL Research University , CNRS UMR 3348, INSERM U1278, Orsay , France

4. Université Paris-Saclay , CNRS UMR 3348, INSERM U1278, Orsay , France

5. Equipe labellisée Ligue contre le Cancer , Orsay , France

Abstract

Abstract Amino acid bioavailability impacts mRNA translation in a codon-dependent manner. Here, we report that the anti-cancer MAPK inhibitors (MAPKi) decrease the intracellular concentration of aspartate and glutamate in melanoma cells. This coincides with the accumulation of ribosomes on codons corresponding to these amino acids and triggers the translation-dependent degradation of mRNAs encoding aspartate- and glutamate-rich proteins, involved in DNA metabolism such as DNA replication and repair. Consequently, cells that survive MAPKi degrade aspartate and glutamate likely to generate energy, which simultaneously decreases their requirement for amino acids due to the downregulation of aspartate- and glutamate-rich proteins involved in cell proliferation. Concomitantly, the downregulation of aspartate- and glutamate-rich proteins involved in DNA repair increases DNA damage loads. Thus, DNA repair defects, and therefore mutations, are at least in part a secondary effect of the metabolic adaptation of cells exposed to MAPKi.

Funder

INCa

Conseil Régional Auvergne Rhône-Alpes

European Research Council

European Union's Horizon 2020

Publisher

Oxford University Press (OUP)

Link

https://academic.oup.com/narcancer/article-pdf/6/2/zcae019/57360144/zcae019.pdf

Reference86 articles.

1. Translation and mRNA stability control;Wu;Annu. Rev. Biochem.,2023

2. Ribosome slowdown triggers codon-mediated mRNA decay independently of ribosome quality control;Mishima;EMBO J.,2022

3. Codon optimality-mediated mRNA degradation: linking translational elongation to mRNA stability;Bae;Mol. Cell,2022

4. Ribosome dynamics and mRNA turnover, a complex relationship under constant cellular scrutiny;Morris;Wiley Interdiscip. Rev. RNA,2021

5. Translation affects mRNA stability in a codon-dependent manner in human cells;Wu;eLife,2019