Pharmacokinetics of colistin methanesulphonate and colistin in rats following an intravenous dose of colistin methanesulphonate

doi:10.1093/jac/dkh167

JAC Advance Access originally published online on March 24, 2004

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Journal of Antimicrobial Chemotherapy (2004) 53, 837-840
© 2004 The British Society for Antimicrobial Chemotherapy

Pharmacokinetics of colistin methanesulphonate and colistin in rats following an intravenous dose of colistin methanesulphonate

Jian Li¹^,2, Robert W. Milne¹, Roger L. Nation²^,*, John D. Turnidge³, Timothy C. Smeaton⁴ and Kingsley Coulthard⁵

¹ Centre for Pharmaceutical Research and ⁴ School of Pharmaceutical, Molecular and Biomedical Sciences, University of South Australia, Adelaide; ² Facility for Anti-infective Drug Development and Innovation, Victorian College of Pharmacy, Monash University, Parkville, Melbourne, Vic 3052; ³ Department of Microbiology and Infectious Diseases and ⁵ Department of Pharmacy, Women’s and Children’s Hospital, North Adelaide, Australia

Received 7 May 2003, returned 21 July 2003; revised 3 February 2004; accepted 5 February 2004

Objectives: To determine the disposition of colistin methanesulphonate(CMS) and colistin following intravenous (iv) administrationof CMS in rats.

Methods: Five rats received a single iv bolus of 15 mg/kg CMS.Plasma concentrations of CMS and of colistin formed by the hydrolysisof CMS were determined by HPLC. The pharmacokinetic parametersof CMS and colistin were calculated using non-compartmentalanalysis.

Results: Total body clearance, volume of distribution at steadystate and terminal half-life of CMS averaged 11.7 mL/min/kg,299 mL/kg and 23.6 min, respectively. The mean terminal half-lifeof colistin was 55.7 min. Approximately 60% of the dose waseliminated via the urine in 24 h and presented as a mixtureof CMS and colistin.

Conclusions: Colistin appeared in plasma soon after administrationof CMS, indicating rapid conversion of CMS into colistin. CMShad a shorter terminal half-life than did colistin, indicatingthat the disposition of the colistin generated from CMS wasrate-limited by its elimination. Most of the dose was recoveredin urine, half in the form of colistin. The high percentageof colistin recovered in urine was believed to be formed byhydrolysis of CMS in the bladder and in the collection vessel,and/or conversion from CMS in the kidney.

Keywords: antibacterials, HPLC, Pseudomonas aeruginosa

^* Corresponding author. Tel: +61-3-9903-9061; Fax: +61-3-9903-9629;E-mail: Roger.Nation{at}vcp.monash.edu.au

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