1. Enterococcus faecalis aggregation substance promotes opsonin-independent binding to human neutrophils via a complement receptor type 3-mediated mechanism
- Author
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M. Michele Mariscalco, Robert M. Rakita, Gary M. Dunny, Natalie N. Vanek, Karen Jacques-Palaz, and Scott I. Simon
- Subjects
Microbiology (medical) ,biology ,CD47 ,Immunology ,Integrin ,General Medicine ,Complement receptor ,medicine.disease ,biology.organism_classification ,Microbiology ,Enterococcus faecalis ,Infectious Diseases ,medicine ,biology.protein ,Immunology and Allergy ,Receptor ,Opsonin ,Selectin ,Leukocyte adhesion deficiency - Abstract
Enterococcus faecalis aggregation substance (AS) mediates efficient adhesion between bacteria, thereby facilitating plasmid exchange as an integral part of a bacterial sex pheromone system. We examined the interaction of AS-bearing E. faecalis with human neutrophils (PMNs), an important component of the host defense system. AS promoted a markedly increased opsonin-independent bacterial binding to PMNs. Adhesion was dependent on the expression of the enterococcal Asc10 protein, which contains two Arg-Gly-Asp (RGD) sequences, and addition of exogenous RGD-containing peptides inhibited AS-mediated binding by 66%. AS-mediated adhesion was inhibited by 85% by anti-human complement receptor type 3 (CR3) monoclonal antibodies or by use of PMNs from a patient with leukocyte adhesion deficiency. However, AS-bearing E. faecalis cells were unable to bind to CHO-Mac-1 cells, expressing functionally active CR3, suggesting the potential need for additional PMN surface receptors for bacterial adhesion. Monoclonal antibodies against integrin-associated protein (CD47) and L -selectin, both of which may interact with CR3 and bind to ligands on E. faecalis , also inhibited AS-dependent binding. The non-opsonic binding of E. faecalis to PMNs may play an important role in this organism’s pathogenesis.
- Published
- 1999
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