Distinct Molecular Features of NleG Type 3 Secreted Effectors Allow for Different Roles during Citrobacter rodentium Infection in Mice.

The NleGs are the largest family of type 3 secreted effectors in attaching and effacing (A/E) pathogens, such as enterohemorrhagic Escherichia coli (EHEC), enteropathogenic E. coli, and Citrobacter rodentium. NleG effectors contain a conserved C-terminal U-box domain acting as a ubiquitin protein ligase and target host proteins via a variable N-terminal portion. The specific roles of these effectors during infection remain uncertain. Here, we demonstrate that the three NleG effectors-NleG1 Cr , NleG7 Cr , and NleG8 Cr -encoded by C. rodentium DBS100 play distinct roles during infection in mice. Using individual nleG Cr knockout strains, we show that NleG7 Cr contributes to bacterial survival during enteric infection while NleG1 Cr promotes the expression of diarrheal symptoms and NleG8 Cr contributes to accelerated lethality in susceptible mice. Furthermore, the NleG8 Cr effector contains a C-terminal PDZ domain binding motif that enables interaction with the host protein GOPC. Both the PDZ domain binding motif and the ability to engage with host ubiquitination machinery via the intact U-box domain proved to be necessary for NleG8 Cr function, contributing to the observed phenotype during infection. We also establish that the PTZ binding motif in the EHEC NleG8 (NleG8 Ec ) effector, which shares 60% identity with NleG8 Cr , is engaged in interactions with human GOPC. The crystal structure of the NleG8 Ec C-terminal peptide in complex with the GOPC PDZ domain, determined to 1.85 Å, revealed a conserved interaction mode similar to that observed between GOPC and eukaryotic PDZ domain binding motifs. Despite these common features, nleG8 Ec does not complement the Δ nleG8 Cr phenotype during infection, revealing functional diversification between these NleG effectors.