Cancers (Oct 2022)

c-MYC Protein Stability Is Sustained by MAPKs in Colorectal Cancer

  • Martina Lepore Signorile,
  • Valentina Grossi,
  • Candida Fasano,
  • Giovanna Forte,
  • Vittoria Disciglio,
  • Paola Sanese,
  • Katia De Marco,
  • Francesca La Rocca,
  • Raffaele Armentano,
  • Anna Maria Valentini,
  • Gianluigi Giannelli,
  • Cristiano Simone

DOI
https://doi.org/10.3390/cancers14194840
Journal volume & issue
Vol. 14, no. 19
p. 4840

Abstract

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c-MYC is one of the most important factors involved in colorectal cancer (CRC) initiation and progression; indeed, it is found to be upregulated in up to 80% of sporadic cases. During colorectal carcinogenesis, c-MYC is maintained upregulated through β-catenin-mediated transcriptional activation and ERK-mediated post-translational stabilization. Our data demonstrate that p38α, a kinase involved in CRC metabolism and survival, contributes to c-Myc protein stability. Moreover, we show that p38α, like ERK, stabilizes c-MYC protein levels by preventing its ubiquitination. Of note, we found that p38α phosphorylates c-MYC and interacts with it both in vitro and in cellulo. Extensive molecular analyses in the cellular and in vivo models revealed that the p38α kinase inhibitors, SB202190 and ralimetinib, affect c-MYC protein levels. Ralimetinib also exhibited a synthetic lethality effect when used in combination with the MEK1 inhibitor trametinib. Overall, our findings identify p38α as a promising therapeutic target, acting directly on c-MYC, with potential implications for countering c-MYC-mediated CRC proliferation, metastatic dissemination, and chemoresistance.

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