The roles of the site-2 protease Eep in Staphylococcus aureus.

In Enterococcus faecalis, the site-2 protease Eep generates sex pheromones, including cAM373. Intriguingly, in Staphylococcus aureus, a peptide similar to cAM373, named cAM373_SA, is produced from the camS gene. Here, we report that the staphylococcal Eep homolog is not only responsible for the production of cAM373_SA but also critical for staphylococcal virulence. As with other Eep proteins, the staphylococcal Eep protein has four transmembrane domain (TM) with the predicted zinc metalloprotease active site (HExxH) in the first TM. The eep deletion reduced the cAM373_SA activity in the culture supernatant to the level of the camS deletion mutant. It also markedly decreased the cAM373 peptide peak in an HPLC analysis. Proteomics analysis showed that Eep affects the production and/or the release of diverse proteins including the signal peptidase subunit SpsB and the surface proteins SpA, SasG, and FnbA. The eep-deletion decreased the adherence of S. aureus to host epithelial cells; however, the adherence of the eep mutant was increased by overexpression of the surface proteins SpA, SasG and FnbA. The eep-deletion reduced the staphylococcal resistance to the killing by human neutrophils as well as the survival in a murine model of blood infection. The overexpression of the surface protein SpA in the eep mutant increased the bacterial survival in the liver. Our study illustrates that, in S. aureus, Eep not only generates cAM373_SA, but also contributes to the survival of the bacterial pathogen in the host.IMPORTANCE The emergence of multi-drug resistant Staphylococcus aureus makes the treatment of staphylococcal infections much more difficult. S. aureus can acquire a drug-resistance gene from other bacteria, such as Enterococcus faecalis. Intriguingly, S. aureus produces a sex pheromone for the E. faecalis plasmid pAM373, raising the possibility that S. aureus might actively promote plasmid conjugation from E. faecalis. In this study, we found that the staphylococcal Eep protein is responsible for the sex pheromone processing and contributes to the survival of the bacteria in the host. These results will enhance future research on the drug resistance acquisition of S. aureus and can lead to the development of novel anti-virulence drugs.