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Infect. Immun., Sep 1997, 3600-3605, Vol 65, No. 9
JF Timoney, SC Artiushin and JS Boschwitz
Streptococcus equi (Streptococcus equi subsp. equi), a Lancefield group C
streptococcus, causes strangles, a highly contagious purulent lymphadenitis
and pharyngitis of members of the family Equidae. The antiphagocytic 58-kDa
M-like protein SeM is a major virulence factor and protective antigen. The
amino acid sequence and structure of SeM has been determined and compared
to that of a second, 40-kDa M-like protein (SzPSe) of S. equi and to those
of other streptococcal proteins. Both SeM and SzPSe are mainly
alpha-helical fibrillar molecules with no homology other than that between
their signal and membrane anchor sequences and are only distantly related
to other streptococcal M and M-like proteins. The sequence of SzPSe
indicates that it is an allele of SzP that encodes the variable protective
M-like and typing antigens of S. zooepidemicus (S. equi subsp.
zooepidemicus). SeM is opsonogenic for S. equi but not for the closely
related S. zooepidemicus, whereas SzPSe is strongly opsonogenic for S.
zooepidemicus but not for S. equi. Both proteins bind equine fibrinogen.
SeM and SzPSe proteins from temporally and geographically separated
isolates of S. equi are identical in size. The results taken together
support previous evidence that S. equi is a clonal pathogen originating
from an ancestral strain of S. zooepidemicus. We postulate that acquisition
of SeM synthesis was a key element in the success of the clone because of
its effect in enhancing resistance to phagocytosis and because protective
immunity entails a requirement for SeM-specific antibody.
Copyright © 1997, American Society for Microbiology
Comparison of the sequences and functions of Streptococcus equi M-like proteins SeM and SzPSe
Gluck Equine Research Center, University of Kentucky, Lexington 40546- 0099, USA.
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