Substantial Targeting Advantage Achieved by Pulmonary Administration of Colistin Methanesulfonate in a Large-Animal Model

Cornelia B Landersdorfer; Tri-Hung Nguyen; Linh Thuy Lieu; Gary Nguyen; Robert J Bischof; Els N Meeusen; Jian Li; Roger L Nation; Michelle P McIntosh

doi:10.1128/AAC.01934-16

Substantial Targeting Advantage Achieved by Pulmonary Administration of Colistin Methanesulfonate in a Large-Animal Model

Antimicrob Agents Chemother. 2016 Dec 27;61(1):e01934-16. doi: 10.1128/AAC.01934-16. Print 2017 Jan.

Authors

Cornelia B Landersdorfer^{1

2

3}, Tri-Hung Nguyen⁴, Linh Thuy Lieu⁴, Gary Nguyen⁵, Robert J Bischof^{5

6}, Els N Meeusen⁵, Jian Li⁴, Roger L Nation⁴, Michelle P McIntosh¹

Affiliations

¹ Drug Delivery, Disposition and Dynamics, Monash Institute of Pharmaceutical Sciences, Monash University, Melbourne, Australia cornelia.landersdorfer@monash.edu michelle.mcintosh@monash.edu.
² Centre for Medicine Use and Safety, Faculty of Pharmacy and Pharmaceutical Sciences, Monash University, Melbourne, Australia.
³ Department of Pharmaceutical Sciences, State University of New York at Buffalo, Buffalo, NY, USA.
⁴ Drug Delivery, Disposition and Dynamics, Monash Institute of Pharmaceutical Sciences, Monash University, Melbourne, Australia.
⁵ Biotechnology Research Laboratories, School of Biomedical Science, Monash University, Clayton, Australia.
⁶ The Ritchie Centre, Hudson Institute of Medical Research, Melbourne, Australia.

Abstract

Colistin, administered as its inactive prodrug colistin methanesulfonate (CMS), is often used in multidrug-resistant Gram-negative pulmonary infections. The CMS and colistin pharmacokinetics in plasma and epithelial lining fluid (ELF) following intravenous and pulmonary dosing have not been evaluated in a large-animal model with pulmonary architecture similar to that of humans. Six merino sheep (34 to 43 kg body weight) received an intravenous or pulmonary dose of 4 to 8 mg/kg CMS (sodium) or 2 to 3 mg/kg colistin (sulfate) in a 4-way crossover study. Pulmonary dosing was achieved via jet nebulization through an endotracheal tube cuff. CMS and colistin were quantified in plasma and bronchoalveolar lavage fluid (BALF) samples by high-performance liquid chromatography (HPLC). ELF concentrations were calculated via the urea method. CMS and colistin were comodeled in S-ADAPT. Following intravenous CMS or colistin administration, no concentrations were quantifiable in BALF samples. Elimination clearance was 1.97 liters/h (4% interindividual variability) for CMS (other than conversion to colistin) and 1.08 liters/h (25%) for colistin. On average, 18% of a CMS dose was converted to colistin. Following pulmonary delivery, colistin was not quantifiable in plasma and CMS was detected in only one sheep. Average ELF concentrations (standard deviations [SD]) of formed colistin were 400 (243), 384 (187), and 184 (190) mg/liter at 1, 4, and 24 h after pulmonary CMS administration. The population pharmacokinetic model described well CMS and colistin in plasma and ELF following intravenous and pulmonary administration. Pulmonary dosing provided high ELF and low plasma colistin concentrations, representing a substantial targeting advantage over intravenous administration. Predictions from the pharmacokinetic model indicate that sheep are an advantageous model for translational research.

Keywords: colistin; intravenous administration; pulmonary administration; pulmonary pharmacokinetics; sheep; systemic pharmacokinetics.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Administration, Inhalation
Administration, Intravenous
Animals
Anti-Bacterial Agents / blood
Anti-Bacterial Agents / pharmacokinetics*
Bronchoalveolar Lavage Fluid / chemistry
Colistin / analogs & derivatives*
Colistin / blood
Colistin / pharmacokinetics*
Cross-Over Studies
Drug Administration Schedule
Drug Dosage Calculations
Humans
Lung / metabolism*
Models, Statistical*
Nebulizers and Vaporizers
Sheep

Substances

Anti-Bacterial Agents
colistinmethanesulfonic acid
Colistin