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Publication : The concomitant loss of APC and HNF4α in adult hepatocytes does not contribute to hepatocarcinogenesis driven by β-catenin activation.

First Author  Sartor C Year  2019
Journal  Liver Int Volume  39
Issue  4 Pages  727-739
PubMed ID  30721564 Mgi Jnum  J:294462
Mgi Id  MGI:6456520 Doi  10.1111/liv.14068
Citation  Sartor C, et al. (2019) The concomitant loss of APC and HNF4alpha in adult hepatocytes does not contribute to hepatocarcinogenesis driven by beta-catenin activation. Liver Int 39(4):727-739
abstractText  BACKGROUND & AIMS: Loss of hepatocyte nuclear factor-4alpha (HNF4alpha), a critical factor driving liver development and differentiation, is frequently associated with hepatocellular carcinoma (HCC). Our recent data revealed that HNF4alpha level was decreased in mouse and human HCCs with activated beta-catenin signalling. In addition, increasing HNF4alpha level by miR-34a inhibition slowed tumour progression of beta-catenin-activated HCC in mice. METHODS: We generated a Hnf4a(flox/flox/) Apc(flox/flox) /TTR-Cre(ERT) (2) (Hnf4a/Apc(Hep) ) mouse line and evaluated the impact of Hnf4a disruption on HCC development and liver homoeostasis. RESULTS: There was no significant impact of Hnf4a disruption on tumour onset and progression in Apc(Hep) model. However, we observed an unexpected phenotype in 28% of Hnf4a(Hep) mice maintained in a conventional animal facility, which presented disorganized portal triads, characterized by stenosis of the portal vein and increased number and size of hepatic arteries and bile ducts. These abnormal portal structures resemble the human idiopathic non-cirrhotic portal hypertension syndrome. We correlated the presence of portal remodelling with a higher expression of protein and mRNA levels of TGFbeta and BMP7, a key regulator of the TGFbeta-dependent endothelial-to-mesenchymal transition. CONCLUSION: These data demonstrate that HNF4alpha does not play a major role during beta-catenin-driven HCC, thus revealing that the tumour suppressor role of HNF4alpha is far more complex and dependent probably on its temporal expression and tumour context. However, HNF4alpha loss in adult hepatocytes could induce abnormal portal structures resembling the human idiopathic non-cirrhotic portal hypertension syndrome, which may result from endothelial- and epithelial-to-mesenchymal transitions.
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