Affiliation:
1. Department of Pediatrics
2. Committee on Microbiology
3. Committee on Molecular Medicine, The University of Chicago, Chicago, Illinois 60637
Abstract
ABSTRACT
We found an increased abundance of
pbpB
-specific transcripts in vancomycin intermediate-resistant
Staphylococcus aureus
(VISA) isolates compared with that found in paired, genetically identical, susceptible isolates. This difference in expression cannot be explained by differences in the
pbpB
promoter sequence. Since the factors controlling
pbpB
gene expression have remained largely unexplored, various conditions that might affect
pbpB
transcript abundance were examined. In both vancomycin-susceptible and VISA strains,
pbpB
expression varied with the growth phase, with the highest abundance of
pbpB
-specific transcripts detected during mid-log phase. Interestingly, both vancomycin and oxacillin were able to induce
pbpB
transcription above a constitutive level. When vancomycin was absent, one of the three
pbpB
-specific transcripts that were usually faintly detected in non-VISA strains was more readily detected in VISA strains during mid-log but not stationary phase. This transcript was enhanced in non-VISA strains by vancomycin induction. Gel shift assays indicated that an increased amount of the putative transcription factor that binds to both P1 and P1′ promoter regions is present in the cytosol of vancomycin-induced cells. Neither the SigB sigma factor nor the quorum-sensing
agr
locus was required for growth phase-variable
pbpB
expression or transcriptional induction of
pbpB
by vancomycin or oxacillin. Also, MecI, MecR1, BlaI, and BlaR1, regulatory proteins that mediate β-lactam-inducible expression of
mecA
and β-lactamase, were not required for antibiotic induction of
pbpB
transcription. These data support the idea that
pbpB
expression is modulated by a
trans
-acting factor in response to the presence of the cell wall-active antibiotics vancomycin and oxacillin.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Pharmacology (medical),Pharmacology
Cited by
40 articles.
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