4.5 Article

Bacteroides fragilis ubiquitin homologue drives intraspecies bacterial competition in the gut microbiome

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NATURE MICROBIOLOGY
Volume -, Issue -, Pages -

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NATURE PORTFOLIO
DOI: 10.1038/s41564-023-01541-5

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In this study, it was discovered that the gut symbiont Bacteroides fragilis secretes a toxic substance called BfUbb that lyses specific B. fragilis strains by binding and inactivating an essential peptidyl-prolyl isomerase (PPIase). The sensitivity of B. fragilis strains to BfUbb was found to be influenced by a specific tyrosine residue in the PPIase. The findings also suggest that BfUbb confers a competitive advantage for encoding strains.
Interbacterial antagonism and associated defensive strategies are both essential during bacterial competition. The human gut symbiont Bacteroides fragilis secretes a ubiquitin homologue (BfUbb) that is toxic to a subset of B. fragilis strains in vitro. In the present study, we demonstrate that BfUbb lyses certain B. fragilis strains by non-covalently binding and inactivating an essential peptidyl-prolyl isomerase (PPIase). BfUbb-sensitivity profiling of B. fragilis strains revealed a key tyrosine residue (Tyr119) in the PPIase and strains that encode a glutamic acid residue at Tyr119 are resistant to BfUbb. Crystal structural analysis and functional studies of BfUbb and the BfUbb-PPIase complex uncover a unique disulfide bond at the carboxy terminus of BfUbb to mediate the interaction with Tyr119 of the PPIase. In vitro coculture assays and mouse studies show that BfUbb confers a competitive advantage for encoding strains and this is further supported by human gut metagenome analyses. Our findings reveal a previously undescribed mechanism of bacterial intraspecies competition.

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