Abstract
Staphylococcus aureus is a prominent bacterial pathogen that is known to agglutinate in the presence of human plasma to form stable clumps. There is increasing evidence that agglutination aids S. aureus pathogenesis, but the mechanisms of this process remain to be fully elucidated. To better define this process, we developed both tube based and flow cytometry methods to monitor clumping in the presence of extracellular matrix proteins. We discovered that the ArlRS two-component system regulates the agglutination mechanism during exposure to human plasma or fibrinogen. Using divergent S. aureus strains, we demonstrated that arlRS mutants are unable to agglutinate, and this phenotype can be complemented. We found that the ebh gene, encoding the Giant Staphylococcal Surface Protein (GSSP), was up-regulated in an arlRS mutant. By introducing an ebh complete deletion into an arlRS mutant, agglutination was restored. To assess whether GSSP is the primary effector, a constitutive promoter was inserted upstream of the ebh gene on the chromosome in a wildtype strain, which prevented clump formation and demonstrated that GSSP has a negative impact on the agglutination mechanism. Due to the parallels of agglutination with infective endocarditis development, we assessed the phenotype of an arlRS mutant in a rabbit combined model of sepsis and endocarditis. In this model the arlRS mutant displayed a large defect in vegetation formation and pathogenesis, and this phenotype was partially restored by removing GSSP. Altogether, we have discovered that the ArlRS system controls a novel mechanism through which S. aureus regulates agglutination and pathogenesis.
Highlights
Staphylococcus aureus is a Gram-positive opportunistic pathogen that exists as part of the normal human microflora in approximately one third of the human population [1]
Staphylococcus aureus is a bacterial pathogen that is responsible for causing significant disease in humans
It has long been recognized that S. aureus can bind human matrix proteins to form stable clumps in a process called agglutination, but the importance of agglutination during infection is only just becoming understood
Summary
Staphylococcus aureus is a Gram-positive opportunistic pathogen that exists as part of the normal human microflora in approximately one third of the human population [1]. This pathogen is responsible for causing a wide range of acute and chronic infections resulting in significant morbidity and mortality in both the hospital and community settings. Biofilms can be defined as a community of cells encased in a protective matrix containing eDNA, proteins, and polysaccharides that are attached to a surface This survival mechanism provides an increased capacity for bacteria to persist in hostile environments created by exposure to antibiotics and host immune defenses [5,7,8]
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