M Protein, a Classical Bacterial Virulence Determinant, Forms Complexes with Fibrinogen That Induce Vascular Leakage

Overview

Journal Cell

Publisher Cell Press

Specialty Cell Biology

Date 2004 Mar 16

PMID 15016372

Citations 133

Authors

Heiko Herwald

Henning Cramer

Matthias Morgelin

Wayne Russell

Ulla Sollenberg

Anna Norrby-Teglund

Hans Flodgaard

Lennart Lindbom

Lars Bjorck

Affiliations

Soon will be listed here.

Abstract

Increased vascular permeability is a key feature of inflammatory conditions. In severe infections, leakage of plasma from the vasculature induces a life-threatening hypotension. Streptococcus pyogenes, a major human bacterial pathogen, causes a toxic shock syndrome (STSS) characterized by excessive plasma leakage and multi-organ failure. Here we find that M protein, released from the streptococcal surface, forms complexes with fibrinogen, which by binding to beta2 integrins of neutrophils, activate these cells. As a result, neutrophils release heparin binding protein, an inflammatory mediator inducing vascular leakage. In mice, injection of M protein or subcutaneous infection with S. pyogenes causes severe pulmonary damage characterized by leakage of plasma and blood cells. These lesions were prevented by treatment with a beta2 integrin antagonist. In addition, M protein/fibrinogen complexes were identified in tissue biopsies from a patient with necrotizing fasciitis and STSS, further underlining the pathogenic significance of such complexes in severe streptococcal infections.

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