Affiliation:
1. Bernhard Nocht Institute for Tropical Medicine, Hamburg, Germany.
Abstract
M protein, the major virulence factor of group A streptococci, has antiopsonic activity in that it inhibits activation of the alternative complement pathway on the streptococcal surface. Two properties of M protein have been claimed to account for the inhibitory activity, namely, (i) its binding affinity for complement factor H, which is an inhibitor of alternative pathway activation, and (ii) its high binding affinity for fibrinogen. We have recently shown that fibrinogen, like M protein, inhibits alternative pathway activation by possessing binding affinity for factor H. Here we report that fibrinogen effectively competes with factor H for binding to M protein but retains its own binding affinity for factor H. The presence of fibrinogen did not significantly affect alternative pathway inhibition on the streptococcal surface.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Immunology,Microbiology,Parasitology
Reference28 articles.
1. Selection of group A streptococci rich in M protein from populations poor in M protein;Becker C. G.;Am. J. Pathol.,1964
2. Fibrinogen binding inhibits fixation of the third component of human complement on the surface of groups A, B, C, and G streptococci;Chhatwal G. S.;Microbiol. Immunol.,1985
3. Regulation by membrane sialic acid of 01H-dependent decay-dissociation of amplification C3 convertase of the alternative complement pathway;Fearon D. T.;Proc. Natl. Acad. Sci. USA,1978
4. Streptococcal M6 protein expressed in E. coli. Localization, purification, and comparison with streptococcal-derived M protein;Fischetti V. A.;J. Exp. Med.,1984
5. The (3-activator system: an alternate pathway of complement activation;Gotze O.;J. Exp. Med.,1971
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