Bile Acid Recognition by Mouse Ileal Bile Acid Binding Protein.

ACS Chem Biol

Department of Chemistry, Case Western Reserve University, 10900 Euclid Avenue, Cleveland, Ohio 44106, United States.

Published: December 2017

AI Article Synopsis

  • I-BABP (FABP6) is a protein found in the ileum that may buffer excess bile acids or help regulate bile acid transcription.
  • Researchers studied mouse I-BABP to understand its binding properties and found that the most prevalent mouse bile acid, β-muricholic acid, binds weakly to I-BABP, especially when combined with other bile acids.
  • The study revealed I-BABP shows a strong preference for the combination of cholic acid and chenodeoxycholic acid, suggesting it plays an important role in regulating bile acid signaling beyond just buffering.

Article Abstract

Ileal bile acid binding protein (I-BABP, gene name FABP6) is a component of the bile acid recycling system, expressed in the ileal enterocyte. The physiological role of I-BABP has been hypothesized to be either an intracellular buffering agent to protect against excess intracellular bile acids or separately as a modulator of bile acid controlled transcription. We investigated mouse I-BABP (mI-BABP) to understand the function of this protein family. Here, we studied energetics and site selectivity of binding with physiological bile acids using a combination of isothermal calorimetric analysis and NMR spectroscopy. We found that the most abundant bile acid in the mouse (β-muricholic acid) binds with weak affinity individually and in combination with other bile acids. Further analysis showed that mI-BABP like human I-BABP (hI-BABP) specifically recognizes the conjugated form of cholic acid:chenodeoxycholic acid (CA:CDCA) in a site-selective manner, displaying the highest affinity of any bile acid combination tested. These results indicate that I-BABP specifically recognizes the ligand combination of CDCA and CA, even in a species such as the mouse where CDCA only represents a trace component of the physiological pool. Specific and conserved recognition of the CDCA and CA ligand combination suggests that I-BABP may play a critical role in the regulation of bile acid signaling in addition to its proposed role as a buffering agent.

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Source
http://dx.doi.org/10.1021/acschembio.7b00865DOI Listing

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