Cellular and Molecular Gastroenterology and Hepatology (Jan 2024)

Quantifying Forms and Functions of Enterohepatic Bile Acid Pools in MiceSummary

  • Koichi Sudo,
  • Amber Delmas-Eliason,
  • Shannon Soucy,
  • Kaitlyn E. Barrack,
  • Jiabao Liu,
  • Akshaya Balasubramanian,
  • Chengyi Jenny Shu,
  • Michael J. James,
  • Courtney L. Hegner,
  • Henry D. Dionne,
  • Alex Rodriguez-Palacios,
  • Henry M. Krause,
  • George A. O’Toole,
  • Saul J. Karpen,
  • Paul A. Dawson,
  • Daniel Schultz,
  • Mark S. Sundrud

Journal volume & issue
Vol. 18, no. 6
p. 101392

Abstract

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Backgrounds & Aims: Bile acids (BAs) are core gastrointestinal metabolites with dual functions in lipid absorption and cell signaling. BAs circulate between the liver and distal small intestine (i.e., ileum), yet the dynamics through which complex BA pools are absorbed in the ileum and interact with host intestinal cells in vivo remain poorly understood. Because ileal absorption is rate-limiting in determining which BAs in the intestinal lumen gain access to host intestinal cells and receptors, and at what concentrations, we hypothesized that defining the rates and routes of ileal BA absorption in vivo would yield novel insights into the physiological forms and functions of mouse enterohepatic BA pools. Methods: Using ex vivo mass spectrometry, we quantified 88 BA species and metabolites in the intestinal lumen and superior mesenteric vein of individual wild-type mice, and cage-mates lacking the ileal BA transporter, Asbt/Slc10a2. Results: Using these data, we calculated that the pool of BAs circulating through ileal tissue (i.e., the ileal BA pool) in fasting C57BL/6J female mice is ∼0.3 μmol/g. Asbt-mediated transport accounted for ∼80% of this pool and amplified size. Passive permeability explained the remaining ∼20% and generated diversity. Compared with wild-type mice, the ileal BA pool in Asbt-deficient mice was ∼5-fold smaller, enriched in secondary BA species and metabolites normally found in the colon, and elicited unique transcriptional responses on addition to ex vivo–cultured ileal explants. Conclusions: This study defines quantitative traits of the mouse enterohepatic BA pool and reveals how aberrant BA metabolism can impinge directly on host intestinal physiology.

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