Pharmacodynamic characterization of efflux and topoisomerase IV-mediated fluoroquinolone resistance in  Streptococcus pneumoniae

doi:10.1093/jac/dkf095

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Journal of Antimicrobial Chemotherapy (2002) 50, 211-218
© 2002 The British Society for Antimicrobial Chemotherapy

Pharmacodynamic characterization of efflux and topoisomerase IV-mediated fluoroquinolone resistance in Streptococcus pneumoniae

Karl J. Madaras-Kelly¹^,2^,*, Christopher Daniels², Marissa Hegbloom¹^,2 and Michelle Thompson¹^,2

¹ Veterans Affairs Medical Center, 500 W. Fort Street, Boise, ID 83702; ² College of Pharmacy, Idaho State University, Pocatello, ID, USA

Received 6 August 2001; returned 4 March 2002; revised 15 April 2002; accepted 29 April 2002

Objectives: Most in vitro investigations of fluoroquinoloneresistance involving Streptococcus pneumoniae have describedgenotypic changes in quinolone resistance-determining regions(QRDRs) that occur as the result of exposure to fluoroquinolonesobtained with static antimicrobial concentrations. The objectivesof this study were to determine whether differences exist betweenmoxifloxacin, sparfloxacin and levofloxacin antimicrobial effect(AME) and their ability to select out stepwise mutations withwild-type, efflux-expressing and parC-mediated fluoroquinoloneresistance while simulating the in vivo dosing and pharmacokineticsof the respective agents.

Methods: A one-compartment pharmacodynamic model simulated fluoroquinolonedosing regimens. Duplicate 24 h experiments were carried outin Mueller–Hinton broth with 3% horse blood at 1 x 10⁸cfu/mL. Reserpine (10 mg/L) was added to select experimentsconducted with efflux-expressing strains. AME was expressedas the area under the time–concentration kill curve (AUEC₂₄).Strains expressing increased MIC post-time–concentrationkill curve (TCKC) were evaluated for changes in QRDR.

Results: Moxifloxacin exhibited a greater AME against all isolates.Efflux was generally associated with partial loss of AME forall fluoroquinolones, and levofloxacin retained no AME againstparC-expressing S. pneumoniae. Increased fluoroquinolone MICpost-TCKC was more common with efflux expression. The additionof reserpine was associated with enhanced AME for levofloxacinand moxifloxacin, but was not associated with altered resistanceselection. Isolates recovered post-TCKC from experiments involvingefflux- or parC mutation-containing isolates generally exhibiteda more than four-fold increase in MIC, which was associatedwith commonly reported substitutions in both parC and gyrA.

Conclusion: The results of this study generally indicate thatresistance selection under pharmacodynamic conditions is similarto results reported with static fluoroquinolone concentrations.While moxifloxacin AME was greater than levofloxacin and sparfloxacin,the overall selection of resistant isolates did not differ.

^* Corresponding author. Tel: +1-208-422-1146; Fax: +1-208-422-1147;E-mail: kmk{at}otc.isu.edu

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