Biochemical pharmacology

A gut bacteria-produced bile acid that reduces liver scarring

Updated

Abstract

Administration of allo-LCA at 10 mg/kg/day may protect against liver damage in mice on a high fat/high fructose diet.

  • Allo-LCA functions as both a dual agonist and inverse agonist, affecting intestinal immunity.
  • In vitro, allo-LCA prevents the polarization of certain immune cells, indicating a role in immune regulation.
  • Mice treated with allo-LCA showed improved insulin sensitivity and reduced liver lipid accumulation compared to untreated mice on a high fat/high fructose diet.
  • The liver transcriptomic profile indicated that allo-LCA reversed dysregulation in pathways linked to inflammation and metabolism.
  • Allo-LCA restored bile acid homeostasis and improved adipose tissue function by reducing pro-inflammatory markers.

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