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Infect Immun. 1991 May; 59(5): 1811-1817
Role of M protein in adherence of group A streptococci.
M G Caparon,
D S Stephens,
A Olsén and
J R Scott
Department of Molecular Microbiology, Washington University School of Medicine, St. Louis, Missouri 63110.
ABSTRACT
The role of the M protein in adherence of group A streptococci to human epithelial cells was directly tested by using an isogenic pair of M+ and M- strains. There was no difference between these strains in the number of streptococcal units that adhered to buccal or tonsillar epithelial cells, indicating the following: (i) that adhesins that are not dependent upon M protein expression are present on the surface of group A streptococci and (ii) that the M protein is not the primary streptococcal adherence ligand. However, the M+ strain adhered to tonsillar epithelial cells as aggregates. This aggregation was dependent on the presence of the M protein, since the isogenic M- strain did not clump. The coaggregation of streptococci suggests that the M protein plays an important role in promoting the formation of microcolonies after initial attachment. Binding to fibronectin, a potential epithelial cell receptor for group A streptococci, was also the same for the isogenic M+ and M- strains as well as for an isogenic strain with a regulatory mutation that decreases the expression of M protein. In summary, the M protein is not the primary streptococcal adhesin, nor is it required to orient the streptococcal adhesin and/or fibronectin receptor.
Infect Immun. 1991 May; 59(5): 1811-1817
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Copyright © 1991 by the American Society for Microbiology. All rights reserved.