Abstract

BackgroundThe resistance of cephalosporins is significantly serious in veterinary clinic. In order to inhibit the bacterial resistance production, the mutant selection window (MSW) hypothesis with Escherichia coli (E. coli) ATCC 25922 exposed to cefquinome in an animal tissue-cage model was investigated.ResultsLocalized infection with E. coli was established in piglets, and the infected animals were administrated intramuscularly with various doses and intervals of cefquinome to provide antibiotic concentrations below the MIC99, between the MIC99 and the mutant prevention concentration (MPC), and above the MPC. E. coli lost susceptibility when drug concentrations fluctuated between the lower and upper boundaries of the window, which defined in vitro as the MIC99 (0.06 μg/mL) and the MPC (0.16 μg/mL) respectively. For PK/PD parameters, there were no mutant selection enrichment when T>MIC99 was ≤ 25% or T>MPC was ≥ 50% of administration interval. When T>MIC99 was > 25% and T>MPC was <50% of administration interval, resistance selection was observed. When AUC24 h/MIC99 and AUC24 h/MPC were considered, the mutant selection window extended from 32.84 h to 125.64 h and from 12.83 h to 49.09 h, respectively.ConclusionsThese findings demonstrate that the MSW exists in vivo for time-dependent antimicrobial agents, and its boundaries fit well with those determined in vitro. Maintenance of antimicrobial concentrations above the MPC for > 50% of administration interval is a straightforward way to restrict the acquisition of resistance in this tissue cage model. This situation was achieved with daily intramuscular doses of 1 mg cefquinome/kg body weight.

Highlights

  • The resistance of cephalosporins is significantly serious in veterinary clinic

  • Bacteria count in tissue-cage model Two perforated tissue-cages were implanted into each piglet

  • When above 1010 Colony forming unit (CFU) bacteria were injected into an implanted cage, no severe illness or distress occurred during a 10-day observation

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Summary

Introduction

In order to inhibit the bacterial resistance production, the mutant selection window (MSW) hypothesis with Escherichia coli (E. coli) ATCC 25922 exposed to cefquinome in an animal tissue-cage model was investigated. According to a proposed hypothesis, resistant mutants selectively amplify at antibiotic concentrations within the mutant selection window (MSW), drug concentrations between the boundary of MIC99. The mutant selection window hypothesis was initially proposed using agar plate assays [5], and explored in several in vitro or in vivo model [6,7,8,9,10,11]. Cefquinome is a fourth generation broad-spectrum cephalosporin antibiotic, which was developed solely for veterinary use and approved for the treatment of respiratory tract disease, acute mastitis and footrot in cattle, calf septicaemia, respiratory diseases in pigs and metritis-mastitis-agalactia syndrome in sow [12,13]. In order to reduce the occurring of cefquinome resistance and even the resistance gene transmission between herd

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