Literature DB >> 16840432

Clinical significance of overexpression of multiple RND-family efflux pumps in Bacteroides fragilis isolates.

Lilian Pumbwe1, Abraham Chang, Rachel L Smith, Hannah M Wexler.   

Abstract

OBJECTIVES: The aim of the present study was to determine correlation between bmeB efflux pump overexpression and resistance to fluoroquinolones and beta-lactams in Bacteroides fragilis clinical isolates (n = 51) and the effects of broad-spectrum efflux pump inhibitors (EPIs) on the MICs of the test antibiotics.
METHODS: Susceptibility to garenoxacin, levofloxacin, moxifloxacin, cefoxitin and faropenem +/- EPIs (CCCP, MC-207,110, reserpine and verapamil) was determined. Expression of bmeB efflux pumps was measured, topoisomerase genes were sequenced and beta-lactamase production was determined.
RESULTS: Isolates were grouped into categories based on susceptibility patterns, topoisomerase sequence and efflux pump expression. Panel I isolates (19/51, 37.3%) were highly resistant to fluoroquinolones and cefoxitin (resistance to all agents was significantly reduced by EPIs, P < 0.05), had a point mutation in gyrA (C-->T) causing a Ser-82-->Phe substitution, and overexpressed bmeB4 and bmeB15. Panel II isolates (7/51; 13.7%) had intermediate-level resistance to fluoroquinolones and cefoxitin and a GyrA substitution. Panel IIIA isolates (21/51; 41.2%) had intermediate-level fluoroquinolone resistance and high-level cefoxitin resistance [resistance to all agents was significantly reduced by EPIs (P < 0.05)] and overexpressed bmeB4 and bmeB15. Panel IIIB isolates (4/51; 7.8%) had low-level fluoroquinolone resistance and high-level resistance to cefoxitin [cefoxitin resistance was significantly reduced by EPIs (P < 0.05)] and overexpressed bmeB4, bmeB6, bmeB10 and bmeB14. All isolates were beta-lactamase-positive.
CONCLUSIONS: These data suggest that bmeB efflux pump overexpression can (i) cause low- to intermediate-level clinically relevant fluoroquinolone resistance; (ii) be coupled with GyrA substitutions to cause high-level fluoroquinolone resistance; (iii) contribute to high-level clinically relevant resistance to beta-lactams.

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Year:  2006        PMID: 16840432     DOI: 10.1093/jac/dkl278

Source DB:  PubMed          Journal:  J Antimicrob Chemother        ISSN: 0305-7453            Impact factor:   5.790


  16 in total

1.  Temporal interplay between efflux pumps and target mutations in development of antibiotic resistance in Escherichia coli.

Authors:  Renu Singh; Michelle C Swick; Kimberly R Ledesma; Zhen Yang; Ming Hu; Lynn Zechiedrich; Vincent H Tam
Journal:  Antimicrob Agents Chemother       Date:  2012-01-09       Impact factor: 5.191

2.  Efflux pump overexpression in multiple-antibiotic-resistant mutants of Bacteroides fragilis.

Authors:  Lilian Pumbwe; Daniel Glass; Hannah M Wexler
Journal:  Antimicrob Agents Chemother       Date:  2006-09       Impact factor: 5.191

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Review 5.  Origin and proliferation of multiple-drug resistance in bacterial pathogens.

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6.  Transposon mutagenesis of the anaerobic commensal, Bacteroides fragilis, using the EZ::TN5 transposome.

Authors:  Yaligara Veeranagouda; Fasahath Husain; Hannah M Wexler
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8.  Impact of anatomic site on growth, efflux-pump expression, cell structure, and stress responsiveness of Bacteroides fragilis.

Authors:  Lilian Pumbwe; Christopher A Skilbeck; Hannah M Wexler
Journal:  Curr Microbiol       Date:  2007-07-26       Impact factor: 2.188

9.  Presence of quorum-sensing systems associated with multidrug resistance and biofilm formation in Bacteroides fragilis.

Authors:  Lilian Pumbwe; Christopher A Skilbeck; Hannah M Wexler
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Review 10.  Bacteroides: the good, the bad, and the nitty-gritty.

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