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Glucan‐binding proteins are essential for shaping Streptococcus mutans biofilm architecture
Author(s) -
Lynch David J.,
Fountain Tracey L.,
Mazurkiewicz Joseph E.,
Banas Jeffrey A.
Publication year - 2007
Publication title -
fems microbiology letters
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.899
H-Index - 151
eISSN - 1574-6968
pISSN - 0378-1097
DOI - 10.1111/j.1574-6968.2006.00576.x
Subject(s) - biofilm , streptococcus mutans , microbiology and biotechnology , glucan , mutant , virulence , biology , bacteria , extracellular , glucosyltransferases , gene , biochemistry , chemistry , genetics
Glucan plays a central role in sucrose‐dependent biofilm formation by the dental pathogen Streptococcus mutans . This organism synthesizes several proteins capable of binding glucan. These are divided into the glucosyltransferases that catalyze the synthesis of glucan and the nonglucosyltransferase glucan‐binding proteins (Gbps). The biological significance of the Gbps has not been thoroughly defined, but studies suggest that these proteins influence virulence and play a role in maintaining biofilm architecture by linking bacteria and extracellular molecules of glucan. We engineered a panel of Gbp mutants, targeting GbpA, GbpC, and GbpD, in which each gene encoding a Gbp was deleted individually and in combination. These strains were then analyzed by confocal microscopy and the biofilm properties were quantified by the biofilm quantification software comstat . All biofilms produced by mutant strains lost significant depth, but the basis for the reduction in height depended on which particular Gbp was missing. The loss of the cell‐bound GbpC appeared dominant as might be expected based on losing the principal receptor for glucan. The loss of an extracellular Gbp, either GbpA or GbpD, also profoundly changed the biofilm architecture, each in a unique manner.

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