Cancers (Oct 2021)

Mir-21 Suppression Promotes Mouse Hepatocarcinogenesis

  • Marta Correia de Sousa,
  • Nicolas Calo,
  • Cyril Sobolewski,
  • Monika Gjorgjieva,
  • Sophie Clément,
  • Christine Maeder,
  • Dobrochna Dolicka,
  • Margot Fournier,
  • Laurent Vinet,
  • Xavier Montet,
  • Jean-François Dufour,
  • Bostjan Humar,
  • Francesco Negro,
  • Christine Sempoux,
  • Michelangelo Foti

DOI
https://doi.org/10.3390/cancers13194983
Journal volume & issue
Vol. 13, no. 19
p. 4983

Abstract

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The microRNA 21 (miR-21) is upregulated in almost all known human cancers and is considered a highly potent oncogene and potential therapeutic target for cancer treatment. In the liver, miR-21 was reported to promote hepatic steatosis and inflammation, but whether miR-21 also drives hepatocarcinogenesis remains poorly investigated in vivo. Here we show using both carcinogen (Diethylnitrosamine, DEN) or genetically (PTEN deficiency)-induced mouse models of hepatocellular carcinoma (HCC), total or hepatocyte-specific genetic deletion of this microRNA fosters HCC development—contrasting the expected oncogenic role of miR-21. Gene and protein expression analyses of mouse liver tissues further indicate that total or hepatocyte-specific miR-21 deficiency is associated with an increased expression of oncogenes such as Cdc25a, subtle deregulations of the MAPK, HiPPO, and STAT3 signaling pathways, as well as alterations of the inflammatory/immune anti-tumoral responses in the liver. Together, our data show that miR-21 deficiency promotes a pro-tumoral microenvironment, which over time fosters HCC development via pleiotropic and complex mechanisms. These results question the current dogma of miR-21 being a potent oncomiR in the liver and call for cautiousness when considering miR-21 inhibition for therapeutic purposes in HCC.

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