FASEB journal : official publication of the Federation of American Societies for Experimental Biology

Activating the bile acid receptor GPBAR1 reverses liver and blood vessel damage in fatty liver disease in mice

Updated

Abstract

Agonism of the bile acid receptor GPBAR1 using BAR501 reversed liver injury and vascular damage in mouse models of nonalcoholic steatohepatitis (NASH).

  • NASH is linked to heightened risk of cardiovascular diseases and mortality.
  • Exposure to a high-fat and fructose diet (HFD-F) caused vascular damage, indicated by increased thickness of aorta walls and elevated inflammatory gene expression.
  • Treatment with BAR501 led to improvements in liver health and promoted browning of white fat tissue.
  • BAR501 treatment also normalized the expression of genes related to nitric oxide and hydrogen sulfide production, affecting vascular function.
  • The beneficial effects of BAR501 were dependent on the presence of the GPBAR1 receptor.

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