Abstract

Pharmacokinetic–pharmacodynamic (PK/PD) integration and modelling were used to predict dosage schedules of oxytetracycline for two pig pneumonia pathogens, Actinobacillus pleuropneumoniae and Pasteurella multocida. Minimum inhibitory concentration (MIC) and mutant prevention concentration (MPC) were determined in broth and porcine serum. PK/PD integration established ratios of average concentration over 48 h (C av0–48 h)/MIC of 5.87 and 0.27 μg/mL (P. multocida) and 0.70 and 0.85 μg/mL (A. pleuropneumoniae) for broth and serum MICs, respectively. PK/PD modelling of in vitro time–kill curves established broth and serum breakpoint values for area under curve (AUC 0–24 h)/MIC for three levels of inhibition of growth, bacteriostasis and 3 and 4 log10 reductions in bacterial count. Doses were then predicted for each pathogen, based on Monte Carlo simulations, for: (i) bacteriostatic and bactericidal levels of kill; (ii) 50% and 90% target attainment rates (TAR); and (iii) single dosing and daily dosing at steady‐state. For 90% TAR, predicted daily doses at steady‐state for bactericidal actions were 1123 mg/kg (P. multocida) and 43 mg/kg (A. pleuropneumoniae) based on serum MICs. Lower TARs were predicted from broth MIC data; corresponding dose estimates were 95 mg/kg (P. multocida) and 34 mg/kg (A. pleuropneumoniae).

Highlights

  • The tetracycline group of antimicrobial drugs, discovered in 1948, has consistently had the highest veterinary sales volume of the seven drug classes analysed by UK-VARSS (2014)

  • All P. multocida and A. pleuropneumoniae isolates were derived from EU field cases of pig pneumonia

  • Minimum inhibitory concentrations and mutant prevention concentration (MPC) were determined for six isolates each of P. multocida and A. pleuropneumoniae, and each was determined in broth and pig serum

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Summary

Introduction

The tetracycline group of antimicrobial drugs, discovered in 1948, has consistently had the highest veterinary sales volume of the seven drug classes analysed by UK-VARSS (2014). According to the Clinical Laboratory Standards Institute (CLSI, 2013), whilst tetracycline is the class representative, MIC and breakpoint interpretation for tetracycline apply to oxytetracycline. Several pathogens implicated in pig pneumonia, including mycoplasma species, were shown historically to be susceptible to the actions of oxytetracycline. It has been registered for veterinary use in most European countries and has been in extensive use in farm animals for more than 60 years. It is still a drug of considerable scientific and clinical interest

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