Hepatocyte vitamin D receptor regulates lipid metabolism and mediates experimental diet-induced steatosis.

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RESEARCH PRODUCT

Hepatocyte vitamin D receptor regulates lipid metabolism and mediates experimental diet-induced steatosis.

Milica Bozic Carla Guzmán Sonia Gatius Eloi Garí Carmelo García-monzón Ramiro Jover Jose M. Valdivielso Marta Benet Sonia Sánchez-campos

subject

0301 basic medicine Apolipoprotein E medicine.medical_specialty CD36 Retinoid X receptor Diet High-Fat Calcitriol receptor 03 medical and health sciences Mice Non-alcoholic Fatty Liver Disease Internal medicine medicine Animals Humans Hepatology biology Fatty liver Lipid metabolism medicine.disease Lipid Metabolism Mice Inbred C57BL Disease Models Animal 030104 developmental biology Endocrinology Liver biology.protein Hepatocytes Receptors Calcitriol lipids (amino acids peptides and proteins)Steatosis Steatohepatitis

description

Background & Aims The pathogenesis and progression of non-alcoholic fatty liver disease (NAFLD) is still incompletely understood. Several nuclear receptors play a role in liver lipid metabolism and can promote hepatosteatosis, but the possible role of vitamin D receptor (VDR) in NAFLD has not been investigated. Methods The expression of liver VDR was investigated in apolipoprotein E knockout ( apoE −/− ) mice on a high fat diet, in wild-type mice on methionine and choline deficient diet and in NAFLD patients with hepatosteatosis and non-alcoholic steatohepatitis. The relevance of VDR was assessed in apoE −/− mice by deletion of VDR or paricalcitol treatment and in human HepG2 cells by VDR transfection or silencing. The role of VDR in fibrosis was also determined in VDR knockout mice ( VDR −/− ) treated with thioacetamide. Results Expression of liver VDR was markedly induced in two mouse models of NAFLD, as well as in patients with hepatosteatosis, but decreased in non-alcoholic steatohepatitis. VDR deletion in high fat diet-fed apoE −/− mice protected against fatty liver, dyslipidemia and insulin resistance, and caused a decrease in taurine-conjugated bile acids, but did not influence fibrosis by thioacetamide. apoE −/− VDR −/− mouse livers showed decreased gene expression of CD36 , DGAT2 , C/EBPα and FGF21 , and increased expression of PNPLA2 , LIPIN1 and PGC1α . Treatment of apoE −/− mice on high fat diet with paricalcitol had modest opposite effects on steatosis and gene expression. Finally, this set of genes showed concordant responses when VDR was overexpressed or silenced in HepG2 cells. Conclusions Induced hepatocyte VDR in NAFLD regulates key hepatic lipid metabolism genes and promotes high fat diet-associated liver steatosis. Therapeutic inhibition of liver VDR may reverse steatosis in early NAFLD. Lay summary The amount of vitamin D receptor is induced early in the livers of mice and humans when they develop non-alcoholic fatty liver disease. If the gene for the vitamin D receptor is deleted, hepatic lipid metabolism changes and mice do not accumulate fat in the liver. We conclude that the vitamin D receptor can contribute to the fatty liver disease promoted by a high fat diet.

year	journal	country	edition	language
2015-06-14	Journal of hepatology

10.1016/j.jhep.2016.05.031 https://pubmed.ncbi.nlm.nih.gov/27245430