4.6 Article

Ileal bile acid transporter inhibition in Cyp2c70 KO mice ameliorates cholestatic liver injury

JOURNAL OF LIPID RESEARCH (2022)

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Journal

JOURNAL OF LIPID RESEARCH
Volume 63, Issue 9, Pages -

Publisher

ELSEVIER
DOI: 10.1016/j.jlr.2022.100261

Keywords

Supplementary key words Cytochrome P450; cholesterol 7?-hydroxylase; sterol 12?-hydroxylase; hydrophobicity; detergency; enterohepatic circulation; muricholic acids; chenodeoxycholic acid; biliary cell proliferation

Categories

Biochemistry & Molecular Biology

Funding

  1. National Institute of Diabetes and Digestive and Kidney Diseases [DK047987, DK056239]
  2. Meredith Brown Fund at Emory
  3. Mason Trust Fund
  4. European Association
  5. Doctoral College Metabolic and Cardio-vascular Disease of the Austrian Science Fund [DK-MCD W1226]
  6. NIH [DK047987-28S1, 3389/1-1]
  7. Deutsche Forschungsgemeinschaft (DFG
  8. German Research Foundation) [T32-GM008367]

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This study found that inhibiting the ileal BA transporter can alleviate liver injury in Cyp2c70 KO mice by reducing hepatic inflammation, macrophage infiltration, and biliary cell proliferation. Additionally, reducing hepatic accumulation of bile acids can alleviate liver injury independent of the hydrophobicity of the bile acid pool.
Cyp2c70 is the liver enzyme in rodents responsible for synthesis of the primary 6hydroxylated muricholate bile acid (BA) species. Cyp2c70 KO mice are devoid of protective, hydrophilic muricholic acids, leading to a more human-like BA composition and subsequent cholestatic liver injury. Pharmacological inhibition of the ileal BA transporter (IBAT) has been shown to be therapeutic in cholestatic models. Here, we aimed to determine if IBAT inhibition with SC-435 is protective in Cyp2c70 KO mice. As compared to WT mice, we found male and female Cyp2c70 KO mice exhibited increased levels of serum liver injury markers, and our evaluation of liver histology revealed increased hepatic inflammation, macrophage infiltration, and biliary cell proliferation. We demonstrate serum and histologic markers of liver damage were markedly reduced with SC-435 treatment. Additionally, we show hepatic gene expression in pathways related to immune cell activation and inflammation were significantly upregulated in Cyp2c70 KO mice and reduced to levels indistinguishable from WT with IBAT inhibition. In Cyp2c70 KO mice, the liver BA content was significantly increased, enriched in chenodeoxycholic acid, and more hydrophobic, exhibiting a hydrophobicity index value and red blood cell lysis properties similar to human liver reduced the total hepatic BA levels but did not affect overall hydrophobicity of the liver BAs. These findings suggest that there may be a threshold in the liver for pathological accretion of hydrophobic BAs and reducing hepatic BA accumulation can be sufficient to alleviate liver injury, independent of BA pool hydrophobicity.

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