The pharmacokinetics and i.m. (IM) bioavailability of flumequine (15 mg kg-1) were investigated in healthy pigs and the findings related to published minimal inhibitory concns. (MICs) for susceptible bacteria of animal origin, and to exptl. detd. MICs for susceptible strains of porcine origin. We found MICs for Escherichia coli, Salmonella spp., Pasteurella spp. and Bordetella spp. in the range 0.5 to >64 ?g mL-1 isolated from infected pigs in the Forli area of Italy; only the Pasteurella multocida strains were sensitive (MIC90 = 0.5 ?g mL-1). After i.v. (IV) injection, flumequine was slowly distributed and eliminated (t 1/2? 11.40 ? 0.16 h and t 1/2? 26.35 ? 1.69 h). The distribution vol. at steady state (V dss) was 752.59 ? 84.03 mL kg-1 and clearance (ClB) was 237.19 ? 17.88 mL kg-1 h-1. After IM administration, peak serum concn. (4.99 ? 0.92 ?g mL-1) was reached between the 2nd and the 3rd hour. The results on MIC of isolated bacteria, although only indicative, suggest that the efficacy of flumequine on Gram-neg. bacteria may be impaired by the emergence of less sensitive or resistant strains.

Pharmacodynamics and pharmacokinetics of flumequine in pigs after single intravenous and intramuscular administration / R. Villa, P. Cagnardi, F. Acocella, P. Massi, P. Anfossi, F. Asta, S Carli. - In: THE VETERINARY JOURNAL. - ISSN 1090-0233. - 170:1(2005), pp. 101-107. [10.1016/j.tvjl.2004.05.012]

Pharmacodynamics and pharmacokinetics of flumequine in pigs after single intravenous and intramuscular administration

R. Villa
Primo
;
P. Cagnardi
Secondo
;
F. Acocella;S. Carli
Ultimo
2005

Abstract

The pharmacokinetics and i.m. (IM) bioavailability of flumequine (15 mg kg-1) were investigated in healthy pigs and the findings related to published minimal inhibitory concns. (MICs) for susceptible bacteria of animal origin, and to exptl. detd. MICs for susceptible strains of porcine origin. We found MICs for Escherichia coli, Salmonella spp., Pasteurella spp. and Bordetella spp. in the range 0.5 to >64 ?g mL-1 isolated from infected pigs in the Forli area of Italy; only the Pasteurella multocida strains were sensitive (MIC90 = 0.5 ?g mL-1). After i.v. (IV) injection, flumequine was slowly distributed and eliminated (t 1/2? 11.40 ? 0.16 h and t 1/2? 26.35 ? 1.69 h). The distribution vol. at steady state (V dss) was 752.59 ? 84.03 mL kg-1 and clearance (ClB) was 237.19 ? 17.88 mL kg-1 h-1. After IM administration, peak serum concn. (4.99 ? 0.92 ?g mL-1) was reached between the 2nd and the 3rd hour. The results on MIC of isolated bacteria, although only indicative, suggest that the efficacy of flumequine on Gram-neg. bacteria may be impaired by the emergence of less sensitive or resistant strains.
Flumequine; Parenteral injection; Pharmacodynamics; Pharmacokinetics; Swine
Settore VET/07 - Farmacologia e Tossicologia Veterinaria
Settore VET/09 - Clinica Chirurgica Veterinaria
2005
Article (author)
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/8960
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