| Literature DB >> 26880578 |
Lena Thomer1, Carla Emolo1, Vilasack Thammavongsa1, Hwan Keun Kim1, Molly E McAdow1, Wenqi Yu1, Matthew Kieffer1, Olaf Schneewind2, Dominique Missiakas2.
Abstract
Host immunity against bacteria typically involves antibodies that recognize the microbial surface and promote phagocytic killing. Methicillin-resistant Staphylococcus aureus (MRSA) is a frequent cause of lethal bloodstream infection; however, vaccines and antibody therapeutics targeting staphylococcal surface molecules have thus far failed to achieve clinical efficacy. S. aureus secretes coagulase (Coa), which activates host prothrombin and generates fibrin fibrils that protect the pathogen against phagocytosis by immune cells. Because of negative selection, the coding sequence for the prothrombin-binding D1-D2 domain is highly variable and does not elicit cross-protective immune responses. The R domain, tandem repeats of a 27-residue peptide that bind fibrinogen, is conserved at the C terminus of all Coa molecules, but its functional significance is not known. We show here that the R domain enables bloodstream infections by directing fibrinogen to the staphylococcal surface, generating a protective fibrin shield that inhibits phagocytosis. The fibrin shield can be marked with R-specific antibodies, which trigger phagocytic killing of staphylococci and protect mice against lethal bloodstream infections caused by a broad spectrum of MRSA isolates. These findings emphasize the critical role of coagulase in staphylococcal escape from opsonophagocytic killing and as a protective antigen for S. aureus vaccines.Entities:
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Year: 2016 PMID: 26880578 PMCID: PMC4813671 DOI: 10.1084/jem.20150074
Source DB: PubMed Journal: J Exp Med ISSN: 0022-1007 Impact factor: 14.307