Affiliation:
1. Department of Microbiology and Immunology, University of Arkansas for Medical Sciences, Little Rock, Arkansas 72205
Abstract
ABSTRACT
We previously identified Rbf as an activator for biofilm formation on polystyrene surfaces in
Staphylococcus aureus
strain 8325-4. However, strain 8325-4 contains genetic mutations that may affect biofilm formation. To extend the observation to other strains, we used strain Newman, a weak biofilm producer, and strain UAMS-1, an osteomyelitis clinical strain, in this study. We found that mutations in the chromosomal
rbf
gene did not affect biofilm formation on polystyrene surfaces in these strains, but transformants of these strains carrying a multiple-copy plasmid containing the
rbf
gene formed stronger biofilms than the wild-type strains and the mutant strains. Using the flow cell method, we found that the chromosomal mutation in the
rbf
gene delayed biofilm formation, whereas strains with a plasmid containing the
rbf
gene accelerated biofilm formation in strains Newman and UAMS-1. These results led us to conclude that
rbf
is an activator of biofilm formation in different strains of
S. aureus
, although the degree of activation varies among strains. In a murine model of foreign body infection, the
rbf
mutations in strain Newman, but not in strain UAMS-1, reduced the bacterial survival rate in catheter lumen. However, UAMS-1 carrying multiple copies of
rbf
in a plasmid increased the bacterial survival rate. The animal studies therefore suggest that Rbf has a role in
S. aureus
virulence.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Immunology,Microbiology,Parasitology
Cited by
28 articles.
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