Bioequivalence and population pharmacokinetic modeling of two forms of antibiotic, cefuroxime lysine and cefuroxime sodium, after intravenous infusion in beagle dogs

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Abstract

To investigate the bioequivalence and the population pharmacokinetics of cefuroxime lysine and cefuroxime sodium in healthy beagle dogs. A randomized 2-period crossover design in 18 healthy beagle dogs after receiving 20, 40, and 80mg/kg of cefuroxime lysine or cefuroxime sodium was conducted. A 3-compartment open model was used as the basic model for the population pharmacokinetic study. Both of the antibiotics exhibited dose-proportional pharmacokinetics over the dose range of 2080mg/kg. The mean relative bioavailability of cefuroxime lysine versus cefuroxime sodium was 1.05 (range, 0.71 to 1.42), with a significant difference between males and females. The estimates of population pharmacokinetic of CL, V 1, Q 2, V 2, Q 3, V 3 were 3.74mL/h, 1.70mL, 29.5mL/min, 3.58mL, 0.31mL/min, and 158mL for cefuroxime lysine and 4.10mL/h, 1.00mL, 38.5mL/min, 4.19mL, 0.06mL/min, and 13.6mL for cefuroxime sodium, respectively. The inter-individual variability was determined to be less than 29.1. A linear pharmacokinetic was revealed for cefuroxime lysine and cefuroxime sodium in dogs after intravenous infusion, and the bioequivalence of these forms of the antibiotic was observed with the significant gender-related differences in mean relative bioavailability of cefuroxime lysine versus cefuroxime sodium. © Copyright 2012 Longshan Zhao et al.

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Zhao, L., Li, Q., Li, X., Yin, R., Chen, X., Geng, L., & Bi, K. (2012). Bioequivalence and population pharmacokinetic modeling of two forms of antibiotic, cefuroxime lysine and cefuroxime sodium, after intravenous infusion in beagle dogs. Journal of Biomedicine and Biotechnology, 2012. https://doi.org/10.1155/2012/507294

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