Pharmacodynamics of ceftazidime and meropenem in cerebrospinal fluid: results of population pharmacokinetic modelling and Monte Carlo simulation

doi:10.1093/jac/dkm325

JAC Advance Access published online on September 4, 2007
Journal of Antimicrobial Chemotherapy, doi:10.1093/jac/dkm325

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© The Author 2007. Published by Oxford University Press on behalf of the British Society for Antimicrobial Chemotherapy. All rights reserved. For Permissions, please e-mail: journals.permissions@oxfordjournals.org

Pharmacodynamics of ceftazidime and meropenem in cerebrospinal fluid: results of population pharmacokinetic modelling and Monte Carlo simulation

T. P. Lodise¹^,2^,3, R. Nau⁴, M. Kinzig¹, G. L. Drusano³, R. N. Jones⁵ and F. Sörgel¹^,*

¹ Institute for Biomedical and Pharmaceutical Research, Nürnberg-Heroldsberg, Germany ² Albany College of Pharmacy, Albany, NY, USA ³ Ordway Research Institute, Albany, NY, USA ⁴ University of Göttingen, Göttingen, Germany ⁵ JMI Laboratories, North Liberty, IA, USA

Received 26 February 2007; returned 12 May 2007; revised 23 July 2007; accepted 2 August 2007

^* Corresponding author. Tel: +49-911-518290; Fax: +49-911-5182920; E-mail: ibmp{at}osn.de

Background: Ceftazidime and meropenem are frequently used in the empiricaltreatment of hospital-acquired cerebrospinal fluid (CSF) infections.Although their dispositions in CSF have been described, theability of these agents to achieve critical pharmacodynamictargets against the array of nosocomial CSF Gram-negative bacteriaencountered in practice has not been reported.

Methods: Serum and CSF pharmacokinetic data were obtained from hospitalpatients with external ventricular drains and who received ceftazidimeor meropenem. Concentration–time profiles in serum andCSF were modelled using a three-compartment model with zero-orderinfusion and first-order elimination and transfer. The modelparameters were identified using population pharmacokineticanalysis [Big Non-Parametric Adaptive Grid (BigNPAG)]. A MonteCarlo simulation (9999 subjects) estimated the probability oftarget attainment (PTA) for total drug CSF concentrations at50% and 100% T_>MIC for ceftazidime 2 g intravenously every8 h and meropenem 2 g intravenously every 8 h. The Gram-negativeinfection isolates of the seven most prevalent Gram-negativebacilli from the Meropenem Yearly Susceptibility Test InformationCollection Program were used as a measure of contemporary MICdistribution.

Results: Post-Bayesian measures of bias and precision, observed-predictedplots and R² values were highly acceptable for both drugs. Althoughthe PTA in CSF was approximately one dilution higher for ceftazidimecompared with meropenem at a given MIC value, the cumulativefraction of response (CFR) in CSF against all Gram-negativeswas markedly higher for meropenem when compared with ceftazidimesecondary to the higher occurrence of lower MIC values for meropenem.Both agents had a low CFR against Pseudomonas aeruginosa.

Conclusions: The pharmacodynamics of meropenem was superior to that of ceftazidimeagainst Gram-negative pathogens in the CSF.

Key Words: population PK , CSF , Gram-negative bacteria

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