Agonism for the bile acid receptor GPBAR1 reverses liver and vascular damage in a mouse model of steatohepatitis

Adriana Carino; Silvia Marchianò; Michele Biagioli; Mariarosaria Bucci; Valentina Vellecco; Vincenzo Brancaleone; Chiara Fiorucci; Angela Zampella; Maria Chiara Monti; Eleonora Distrutti; Stefano Fiorucci

doi:10.1096/fj.201801373RR

Agonism for the bile acid receptor GPBAR1 reverses liver and vascular damage in a mouse model of steatohepatitis

FASEB J. 2019 Feb;33(2):2809-2822. doi: 10.1096/fj.201801373RR. Epub 2018 Oct 10.

Affiliations

¹ Department of Surgical and Biomedical Sciences, University of Perugia, Perugia, Italy.
² Department of Pharmacy, University of Naples Federico II, Naples, Italy.
³ Department of Science, University of Basilicata, Potenza, Italy.
⁴ Department of Pharmacy, University of Salerno, Fisciano, Salerno, Italy; and.
⁵ Azienda Ospedaliera di Perugia, Perugia, Italy.

PMID: 30303744
DOI: 10.1096/fj.201801373RR

Abstract

Nonalcoholic steatohepatitis (NASH) is associated with an increased risk of developing cardiovascular complications and mortality, suggesting that treatment of NASH might benefit from combined approaches that target the liver and the cardiovascular components of NASH. Using genetic and pharmacologic approaches, we show that G protein-coupled bile acid-activated receptor 1 (GPBAR1) agonism reverses liver and vascular damage in mouse models of NASH. NASH is associated with accelerated vascular inflammation representing an independent risk factor for development of cardiovascular diseases and cardiovascular-related mortality. GPBAR1, also known as TGR5, is a G protein-coupled receptor for secondary bile acids that reduces inflammation and promotes energy expenditure. Using genetic and pharmacologic approaches, we investigated whether GPBAR1 agonism by 6β-ethyl-3α,7β-dihydroxy-5β-cholan-24-ol (BAR501) reverses liver and vascular damage induced by exposure to a diet enriched in fat and fructose (HFD-F). Treating HFD-F mice with BAR501 reversed liver injury and promoted the browning of white adipose tissue in a Gpbar1-dependent manner. Feeding HFD-F resulted in vascular damage, as shown by the increased aorta intima-media thickness and increased expression of inflammatory genes (IL-6,TNF-α, iNOS, and F4/80) and adhesion molecules (VCAM, intercellular adhesion molecule-1, and endothelial selectin) in the aorta, while reducing the expression of genes involved in NO and hydrogen sulfide generation, severely altering vasomotor activities of aortic rings in an ex vivo assay. BAR501 reversed this pattern in a Gpbar1-dependent manner, highlighting a potential role for GPBAR1 agonism in treating the liver and vascular component of NASH.-Carino, A., Marchianò, S., Biagioli, M., Bucci, M., Vellecco, V., Brancaleone, V., Fiorucci, C., Zampella, A., Monti, M. C., Distrutti, E., Fiorucci, S. Agonism for the bile acid receptor GPBAR1 reverses liver and vascular damage in a mouse model of steatohepatitis.

Keywords: NASH; TGR5; aortic rings; high fat diet.

MeSH terms

Animals
Cholestanols / pharmacology*
Diet, High-Fat / adverse effects
Disease Models, Animal*
Inflammation / etiology
Inflammation / metabolism
Inflammation / pathology
Inflammation / prevention & control*
Liver Diseases / etiology
Liver Diseases / metabolism
Liver Diseases / pathology
Liver Diseases / prevention & control*
Male
Mice
Mice, Inbred C57BL
Mice, Knockout
Non-alcoholic Fatty Liver Disease / etiology
Non-alcoholic Fatty Liver Disease / physiopathology*
Receptors, G-Protein-Coupled / agonists*
Receptors, G-Protein-Coupled / physiology
Vascular Diseases / etiology
Vascular Diseases / metabolism
Vascular Diseases / pathology
Vascular Diseases / prevention & control*

Substances

6-ethyl-3,7-dihydroxycholan-24-ol
Cholestanols
Gpbar1 protein, mouse
Receptors, G-Protein-Coupled