A biosynthetic pathway for the selective sulfonation of steroidal metabolites by human gut bacteria

细菌 生物化学 肠道细菌 生物 肠道菌群 微生物学 化学 遗传学
作者
Lina Yao,Gabriel D. D’Agostino,Jinseok Park,Saiyu Hang,Arijit A. Adhikari,Yancong Zhang,Wei Li,Julián Ávila-Pacheco,Sena Bae,Clary B. Clish,Eric A. Franzosa,Curtis Huttenhower,Jun R. Huh,A. Sloan Devlin
出处
期刊:Nature microbiology [Nature Portfolio]
卷期号:7 (9): 1404-1418 被引量:84
标识
DOI:10.1038/s41564-022-01176-y
摘要

Members of the human gut microbiome enzymatically process many bioactive molecules in the gastrointestinal tract. Most gut bacterial modifications characterized so far are hydrolytic or reductive in nature. Here we report that abundant human gut bacteria from the phylum Bacteroidetes perform conjugative modifications by selectively sulfonating steroidal metabolites. While sulfonation is a ubiquitous biochemical modification, this activity has not yet been characterized in gut microbes. Using genetic and biochemical approaches, we identify a widespread biosynthetic gene cluster that encodes both a sulfotransferase (BtSULT, BT0416) and enzymes that synthesize the sulfonate donor adenosine 3′-phosphate-5′-phosphosulfate (PAPS), including an APS kinase (CysC, BT0413) and an ATP sulfurylase (CysD and CysN, BT0414–BT0415). BtSULT selectively sulfonates steroidal metabolites with a flat A/B ring fusion, including cholesterol. Germ-free mice monocolonized with Bacteroides thetaiotaomicron ΔBT0416 exhibited reduced gastrointestinal levels of cholesterol sulfate (Ch-S) compared with wild-type B. thetaiotaomicron-colonized mice. The presence of BtSULT and BtSULT homologues in bacteria inhibited leucocyte migration in vitro and in vivo, and abundances of cluster genes were significantly reduced in patients with inflammatory bowel disease. Together, these data provide a mechanism by which gut bacteria sulfonate steroidal metabolites and suggest that these compounds can modulate immune cell trafficking in the host. Characterization of a biosynthetic pathway for the sulfonation of steroidal metabolites, such as cholesterol, by gut bacteria may have implications for immune cell trafficking and inflammatory bowel disease.
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