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A Forward Chemical Genetic Screen Reveals Gut Microbiota Metabolites That Modulate Host Physiology.


ABSTRACT: The intestinal microbiota produces tens of thousands of metabolites. Here, we used host sensing of small molecules by G-protein coupled receptors (GPCRs) as a lens to illuminate bioactive microbial metabolites that impact host physiology. We screened 144 human gut bacteria against the non-olfactory GPCRome and identified dozens of bacteria that activated both well-characterized and orphan GPCRs, including strains that converted dietary histidine into histamine and shaped colonic motility; a prolific producer of the essential amino acid L-Phe, which we identified as an agonist for GPR56 and GPR97; and a species that converted L-Phe into the potent psychoactive trace amine phenethylamine, which crosses the blood-brain barrier and triggers lethal phenethylamine poisoning after monoamine oxidase inhibitor administration. These studies establish an orthogonal approach for parsing the microbiota metabolome and uncover multiple biologically relevant host-microbiota metabolome interactions.

SUBMITTER: Chen H 

PROVIDER: S-EPMC6536006 | biostudies-literature | 2019 May

REPOSITORIES: biostudies-literature

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A Forward Chemical Genetic Screen Reveals Gut Microbiota Metabolites That Modulate Host Physiology.

Chen Haiwei H   Nwe Phu-Khat PK   Yang Yi Y   Rosen Connor E CE   Bielecka Agata A AA   Kuchroo Manik M   Cline Gary W GW   Kruse Andrew C AC   Ring Aaron M AM   Crawford Jason M JM   Palm Noah W NW  

Cell 20190418 5


The intestinal microbiota produces tens of thousands of metabolites. Here, we used host sensing of small molecules by G-protein coupled receptors (GPCRs) as a lens to illuminate bioactive microbial metabolites that impact host physiology. We screened 144 human gut bacteria against the non-olfactory GPCRome and identified dozens of bacteria that activated both well-characterized and orphan GPCRs, including strains that converted dietary histidine into histamine and shaped colonic motility; a prol  ...[more]

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