Bile salt hydrolase catalyses formation of amine-conjugated bile acids

Rimal, Bipin and Collins, Stephanie L. and Tanes, Ceylan E. and Rocha, Edson R. and Granda, Megan A. and Solanki, Sumeet and Hoque, Nushrat J. and Gentry, Emily C. and Koo, Imhoi and Reilly, Erin R. and Hao, Fuhua and Paudel, Devendra and Singh, Vishal and Yan, Tingting and Kim, Min Soo and Bittinger, Kyle and Zackular, Joseph P. and Krausz, Kristopher W. and Desai, Dhimant and Amin, Shantu and Coleman, James P. and Shah, Yatrik M. and Bisanz, Jordan E. and Gonzalez, Frank J. and Vanden Heuvel, John P. and Wu, Gary D. and Zemel, Babette S. and Dorrestein, Pieter C. and Weinert, Emily E. and Patterson, Andrew D. (2024) Bile salt hydrolase catalyses formation of amine-conjugated bile acids. Nature, 626 (8000). pp. 859-863. ISSN 0028-0836

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Abstract

Bacteria in the gastrointestinal tract produce amino acid bile acid amidates that can affect host-mediated metabolic processes;however, the bacterial gene(s) responsible for their production remain unknown. Herein, we report that bile salt hydrolase (BSH) possesses dual functions in bile acid metabolism. Specifically, we identified a previously unknown role for BSH as an amine N-acyltransferase that conjugates amines to bile acids, thus forming bacterial bile acid amidates (BBAAs). To characterize this amine N-acyltransferase BSH activity, we used pharmacological inhibition of BSH, heterologous expression of bsh and mutants in Escherichia coli and bsh knockout and complementation in Bacteroides fragilis to demonstrate that BSH generates BBAAs. We further show in a human infant cohort that BBAA production is positively correlated with the colonization of bsh-expressing bacteria. Lastly, we report that in cell culture models, BBAAs activate host ligand-activated transcription factors including the pregnane X receptor and the aryl hydrocarbon receptor. These findings enhance our understanding of how gut bacteria, through the promiscuous actions of BSH, have a significant role in regulating the bile acid metabolic network.

Item Type: Article
Subjects: STM Article > Multidisciplinary
Depositing User: Unnamed user with email support@stmarticle.org
Date Deposited: 23 Feb 2024 06:45
Last Modified: 23 Feb 2024 06:45
URI: http://publish.journalgazett.co.in/id/eprint/1893

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