Fibrin(ogen) engagement of S. aureus promotes the host antimicrobial response and suppression of microbe dissemination following peritoneal infection.

Oscar Negrón,Brian P Conlon,Woosuk S Hur,David S Paul,Sarah E Rowe,Wolfgang Bergmeier,Magnus Hӧӧk,Matthew J Flick,Joni Prasad,Silvio Antoniak,Sara R Abrahams,Jay L Degen,Alice Prince

doi:10.1371/journal.ppat.1010227

Abstract

The blood-clotting protein fibrin(ogen) plays a critical role in host defense against invading pathogens, particularly against peritoneal infection by the Gram-positive microbe Staphylococcus aureus. Here, we tested the hypothesis that direct binding between fibrin(ogen) and S. aureus is a component of the primary host antimicrobial response mechanism and prevention of secondary microbe dissemination from the peritoneal cavity. To establish a model system, we showed that fibrinogen isolated from FibγΔ5 mice, which express a mutant form lacking the final 5 amino acids of the fibrinogen γ chain (termed fibrinogenγΔ5), did not support S. aureus adherence when immobilized and clumping when in suspension. In contrast, purified wildtype fibrinogen supported robust adhesion and clumping that was largely dependent on S. aureus expression of the receptor clumping factor A (ClfA). Following peritoneal infection with S. aureus USA300, FibγΔ5 mice displayed worse survival compared to WT mice coupled to reduced bacterial killing within the peritoneal cavity and increased dissemination of the microbes into circulation and distant organs. The failure of acute bacterial killing, but not enhanced dissemination, was partially recapitulated by mice infected with S. aureus USA300 lacking ClfA. Fibrin polymer formation and coagulation transglutaminase Factor XIII each contributed to killing of the microbes within the peritoneal cavity, but only elimination of polymer formation enhanced systemic dissemination. Host macrophage depletion or selective elimination of the fibrin(ogen) β2-integrin binding motif both compromised local bacterial killing and enhanced S. aureus systemic dissemination, suggesting fibrin polymer formation in and of itself was not sufficient to retain S. aureus within the peritoneal cavity. Collectively, these findings suggest that following peritoneal infection, the binding of S. aureus to stabilized fibrin matrices promotes a local, macrophage-mediated antimicrobial response essential for prevention of microbe dissemination and downstream host mortality.

Highlights

Staphylococcus aureus (S. aureus) is a common, Gram-positive bacterium that colonizes 20– 80% of healthy adults [1]
The contribution of fibrinogen-S. aureus binding through the fibrinogen receptor clumping factor A (ClfA) in peritoneal infection has not been defined
In a mouse model of peritonitis, loss of these activities resulted in diminished bacterial killing, increased bacterial dissemination, and worsened host survival

Summary

Introduction

Staphylococcus aureus (S. aureus) is a common, Gram-positive bacterium that colonizes 20– 80% of healthy adults [1] It is the causative agent for a variety of illnesses ranging from minor skin infections to more serious and life-threatening conditions such as bacteremia, sepsis, infective endocarditis, and pneumonia [2]. S. aureus expresses multiple virulence factors that allow the bacterium to engage and manipulate components of the host coagulation system, including a variety of proteins that directly bind fibrin(ogen). ClfA has been identified as an important factor of S. aureus virulence in animal models of bacteremia, septic arthritis and endocarditis through fibrin(ogen)-dependent and independent mechanisms [7,8,9,10,11]

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