Hepatocyte-Specific Deletion of HIF2α Prevents NASH-Related Liver Carcinogenesis by Decreasing Cancer Cell Proliferation

Beatrice Foglia; Salvatore Sutti; Stefania Cannito; Chiara Rosso; Marina Maggiora; Riccardo Autelli; Erica Novo; Claudia Bocca; Gianmarco Villano; Naresh Naik Ramavath; Ramy Younes; Ignazia Tusa; Elisabetta Rovida; Patrizia Pontisso; Elisabetta Bugianesi; Emanuele Albano; Maurizio Parola

doi:10.1016/j.jcmgh.2021.10.002

Hepatocyte-Specific Deletion of HIF2α Prevents NASH-Related Liver Carcinogenesis by Decreasing Cancer Cell Proliferation

Cell Mol Gastroenterol Hepatol. 2022;13(2):459-482. doi: 10.1016/j.jcmgh.2021.10.002. Epub 2021 Oct 14.

Authors

Beatrice Foglia¹, Salvatore Sutti², Stefania Cannito¹, Chiara Rosso³, Marina Maggiora¹, Riccardo Autelli¹, Erica Novo¹, Claudia Bocca¹, Gianmarco Villano⁴, Naresh Naik Ramavath², Ramy Younes³, Ignazia Tusa⁵, Elisabetta Rovida⁵, Patrizia Pontisso⁴, Elisabetta Bugianesi³, Emanuele Albano², Maurizio Parola⁶

Affiliations

¹ Unit of Experimental Medicine and Clinical Pathology, Department of Clinical and Biological Sciences, University of Turin, Italy.
² Department of Health Sciences and Interdisciplinary Research Centre for Autoimmune Diseases, University Amedeo Avogadro of East Piedmont, Novara, Italy.
³ Department of Medical Sciences, University of Turin, Torino, Italy; Division of Gastroenterology, San Giovanni Hospital, Torino, Italy.
⁴ Department of Medicine, University of Padova, Padova, Italy.
⁵ Unit of Experimental Oncology and Pathology, Department of Experimental and Clinical Biomedical Sciences, University of Florence, Florence, Italy.
⁶ Unit of Experimental Medicine and Clinical Pathology, Department of Clinical and Biological Sciences, University of Turin, Italy. Electronic address: maurizio.parola@unito.it.

Abstract

Background & aims: Hypoxia and hypoxia-inducible factors (HIFs) are involved in chronic liver disease progression. We previously showed that hepatocyte HIF-2α activation contributed significantly to nonalcoholic fatty liver disease progression in experimental animals and human patients. In this study, using an appropriate genetic murine model, we mechanistically investigated the involvement of hepatocyte HIF-2α in experimental nonalcoholic steatohepatitis (NASH)-related carcinogenesis.

Methods: The role of HIF-2α was investigated by morphologic, cellular, and molecular biology approaches in the following: (1) mice carrying hepatocyte-specific deletion of HIF-2α (HIF-2α^-/- mice) undergoing a NASH-related protocol of hepatocarcinogenesis; (2) HepG2 cells stably transfected to overexpress HIF-2α; and (3) liver specimens from NASH patients with hepatocellular carcinoma.

Results: Mice carrying hepatocyte-specific deletion of HIF-2α (hHIF-2α^-/-) showed a significant decrease in the volume and number of liver tumors compared with wild-type littermates. These effects did not involve HIF-1α changes and were associated with a decrease of cell proliferation markers proliferating cell nuclear antigen and Ki67. In both human and rodent nonalcoholic fatty liver disease-related tumors, HIF-2α levels were strictly associated with hepatocyte production of SerpinB3, a mediator previously shown to stimulate liver cancer cell proliferation through the Hippo/Yes-associated protein (YAP)/c-Myc pathway. Consistently, we observed positive correlations between the transcripts of HIF-2α, YAP, and c-Myc in individual hepatocellular carcinoma tumor masses, while HIF-2α deletion down-modulated c-Myc and YAP expression without affecting extracellular signal-regulated kinase 1/2, c-Jun N-terminal kinase, and AKT-dependent signaling. In vitro data confirmed that HIF-2α overexpression induced HepG2 cell proliferation through YAP-mediated mechanisms.

Conclusions: These results indicate that the activation of HIF-2α in hepatocytes has a critical role in liver carcinogenesis during NASH progression, suggesting that HIF-2α-blocking agents may serve as novel putative therapeutic tools.

Keywords: HIF-2α; Hepatocellular Carcinoma; NAFLD; NASH.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Basic Helix-Loop-Helix Transcription Factors / genetics
Basic Helix-Loop-Helix Transcription Factors / metabolism
Carcinogenesis / genetics
Carcinogenesis / metabolism
Carcinoma, Hepatocellular* / pathology
Cell Proliferation
Hepatocytes / metabolism
Humans
Mice
Non-alcoholic Fatty Liver Disease* / metabolism

Substances

Basic Helix-Loop-Helix Transcription Factors