Pharmacokinetics of Gentamicin C 1 , C 1a , and C 2 in Beagles after a Single Intravenous Dose

Author:

Isoherranen Nina12,Lavy Eran3,Soback Stefan1

Affiliation:

1. Kimron Veterinary Institute, Beit Dagan,1 and

2. Laboratory of Analytical Chemistry, Department of Chemistry, University of Helsinki, Helsinki, Finland2

3. Koret School of Veterinary Medicine, Hebrew University of Jerusalem, Jerusalem,3 Israel, and

Abstract

ABSTRACT The pharmacokinetics of gentamicin C 1 , C 2 , and C 1a were studied in six beagles after administration of gentamicin at 4 mg/kg of body weight as a single intravenous bolus dose. Plasma concentrations of the gentamicin components were analyzed with a novel high-performance liquid chromatography method capable of identifying and quantifying each of the components. The pharmacokinetic analysis of the plasma concentration-versus-time data was performed using the noncompartmental approach. The results indicated significant differences in the pharmacokinetic characteristics between the gentamicin components C 1 , C 1a , and C 2 . The mean residence times of gentamicin C 1 , C 1a , and C 2 were 81 ± 13, 84 ± 12, and 79 ± 13 min (mean ± standard deviation), respectively. The half-lives of the respective components were 64 ± 12, 66 ± 12 and 63 ± 12 min. Clearance (CL) of gentamicin C 1 , 4.62 ± 0.71 ml min −1 kg −1 , was significantly higher ( P = 0.0156) than CL of gentamicin C 1a , 1.81 ± 0.26 ml min −1 kg −1 , and C 2 , 1.82 ± 0.25 ml min −1 kg −1 . Similarly, the volume of distribution at steady state ( V ss ) of gentamicin C 1 , 0.36 ± 0.04 liter kg −1 , was significantly higher ( P = 0.0156) than the V ss of gentamicin C 1a , 0.14 ± 0.01 liter kg −1 , and C 2 , 0.15 ± 0.02 liter kg −1 . Tissue binding was considered the most likely cause for the difference. The difference may have clinical and toxicological significance.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

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