EMD-39494

Single-particle
2.97 Å
EMD-39494 Deposition: 18/03/2024
Map released: 25/09/2024
Last modified: 30/10/2024
Overview 3D View Sample Experiment Validation Volume Browser Additional data Links
Overview 3D View Sample Experiment Validation Volume Browser Additional data Links

EMD-39494

Cryo-EM structure of ButCD complex

EMD-39494

Single-particle
2.97 Å
EMD-39494 Deposition: 18/03/2024
Map released: 25/09/2024
Last modified: 30/10/2024
Overview 3D View Sample Experiment Validation Volume Browser Additional data Links
Sample Organism: Bacteroides fragilis
Sample: ButCD complex
Fitted models: 8ypu (Avg. Q-score: 0.606)

Deposition Authors: Xu JH , Chen Z , Gao X
A highly conserved SusCD transporter determines the import and species-specific antagonism of Bacteroides ubiquitin homologues.
Tong M, Xu J, Li W , Jiang K , Yang Y, Chen Z , Jiao X , Meng X, Wang M , Hong J , Long H, Liu SJ , Lim B , Gao X
(2024) Nat Commun , 15 , 8794 - 8794
PUBMED: 39389974
DOI: doi:10.1038/s41467-024-53149-w
ISSN: 2041-1723
Abstract:
Efficient interbacterial competitions and diverse defensive strategies employed by various bacteria play a crucial role in acquiring a hold within a dense microbial community. The gut symbiont Bacteroides fragilis secretes an antimicrobial ubiquitin homologue (BfUbb) that targets an essential periplasmic PPIase to drive intraspecies bacterial competition. However, the mechanisms by which BfUbb enters the periplasm and its potential for interspecies antagonism remain poorly understood. Here, we employ transposon mutagenesis and identify a highly conserved TonB-dependent transporter SusCD (designated as ButCD) in B. fragilis as the BfUbb transporter. As a putative protein-related nutrient utilization system, ButCD is widely distributed across diverse Bacteroides species with varying sequence similarity, resulting in distinct import efficiency of Bacteroides ubiquitin homologues (BUbb) and thereby determining the species-specific toxicity of BUbb. Cryo-EM structural and functional investigations of the BfUbb-ButCD complex uncover distinctive structural features of ButC that are crucial for its targeting by BfUbb. Animal studies further demonstrate the specific and efficient elimination of enterotoxigenic B. fragilis (ETBF) in the murine gut by BfUbb, suggesting its potential as a therapeutic against ETBF-associated inflammatory bowel disease and colorectal cancer. Our findings provide a comprehensive elucidation of the species-specific toxicity exhibited by BUbb and explore its potential applications.