Cellular and Molecular Gastroenterology and Hepatology (Jan 2021)

Cholangiopathy and Biliary Fibrosis in Cyp2c70-Deficient Mice Are Fully Reversed by Ursodeoxycholic AcidSummary

  • Jan Freark de Boer,
  • Hilde D. de Vries,
  • Anna Palmiotti,
  • Rumei Li,
  • Marwah Doestzada,
  • Joanne A. Hoogerland,
  • Jingyuan Fu,
  • Anouk M. La Rose,
  • Marit Westerterp,
  • Niels L. Mulder,
  • Milaine V. Hovingh,
  • Martijn Koehorst,
  • Niels J. Kloosterhuis,
  • Justina C. Wolters,
  • Vincent W. Bloks,
  • Joel T. Haas,
  • David Dombrowicz,
  • Bart Staels,
  • Bart van de Sluis,
  • Folkert Kuipers

Journal volume & issue
Vol. 11, no. 4
pp. 1045 – 1069

Abstract

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Background and Aims: Bile acids (BAs) aid intestinal fat absorption and exert systemic actions by receptor-mediated signaling. BA receptors have been identified as drug targets for liver diseases. Yet, differences in BA metabolism between humans and mice hamper translation of pre-clinical outcomes. Cyp2c70-ablation in mice prevents synthesis of mouse/rat-specific muricholic acids (MCAs), but potential (patho)physiological consequences of their absence are unknown. We therefore assessed age- and gender-dependent effects of Cyp2c70-deficiency in mice. Methods: The consequences of Cyp2c70-deficiency were assessed in male and female mice at different ages. Results: Cyp2c70-/- mice were devoid of MCAs and showed high abundances of chenodeoxycholic and lithocholic acids. Cyp2c70-deficiency profoundly impacted microbiome composition. Bile flow and biliary BA secretion were normal in Cyp2c70-/- mice of both sexes. Yet, the pathophysiological consequences of Cyp2c70-deficiency differed considerably between sexes. Three-week old male Cyp2c70-/- mice showed high plasma BAs and transaminases, which spontaneously decreased thereafter to near-normal levels. Only mild ductular reactions were observed in male Cyp2c70-/- mice up to 8 months of age. In female Cyp2c70-/- mice, plasma BAs and transaminases remained substantially elevated with age, gut barrier function was impaired and bridging fibrosis was observed at advanced age. Addition of 0.1% ursodeoxycholic acid to the diet fully normalized hepatic and intestinal functions in female Cyp2c70-/- mice. Conclusion: Cyp2c70-/- mice show transient neonatal cholestasis and develop cholangiopathic features that progress to bridging fibrosis in females only. These consequences of Cyp2c70-deficiency are restored by treatment with UDCA, indicating a role of BA hydrophobicity in disease development.

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