Evaluation of the predictive performance of four pharmacokinetic models for propofol

doi:10.1093/bja/aep043

BJA Advance Access published online on March 18, 2009
British Journal of Anaesthesia, doi:10.1093/bja/aep043

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© The Author [2009]. Published by Oxford University Press on behalf of The Board of Directors of the British Journal of Anaesthesia. All rights reserved. For Permissions, please email: journals.permissions@oxfordjournal.org

Evaluation of the predictive performance of four pharmacokinetic models for propofol

J. B. Glen¹^,* and F. Servin²

¹ Research Department, Glen Pharma Ltd, 35A Bexton Road, Knutsford, Cheshire, UK
² Department of Anaesthesia, University Hospital Centre, Hopital Bichat, 75877 Paris, France

^* Corresponding author. E-mail: jbg{at}glenpharma.com

Background: This study has compared the predictive performance of four pharmacokineticmodels, two of which are currently incorporated in commercialtarget-controlled infusion pumps for the administration of propofol.

Methods: Arterial propofol concentrations and patient characteristicdata were available from nine patients who, in a published study,had received a standardized infusion of propofol. Predictedconcentrations with ‘Diprifusor’ (Marsh), ‘Schnider’,‘Schuttler’, and ‘White’ models wereobtained by computer simulation. The predictive performanceof each model was assessed overall and over the following phases:rapid infusion (1–5 min), early (1–21 min), maintenance(21-min end-infusion), and recovery (2–20 min post-infusion).

Results: The overall assessment, based on 29–36 samples from eachpatient, indicated that all four models were clinically acceptable.However, the negligible bias (–0.1%) with the ‘Schnider’model was accompanied by overprediction in the rapid infusionphase and underprediction during recovery. This changing biasover time was not detected as ‘divergence’ whenassessed on absolute performance error (APE), (1.4% h^–1)but became significant (13.2% h^–1) when based on changesin signed PE over time. The ‘Schuttler’ model performedwell at most phases but overpredicted concentrations duringrecovery. The White model led to a marginal improvement over‘Diprifusor’ and would be expected to reduce thepositive bias usually seen with ‘Diprifusor’ systems.

Conclusions: In assessing the predictive performance of pharmacokinetic models,additional information can be obtained by analysis of bias atdifferent phases of an infusion. The evaluation of divergenceshould involve linear regression analysis of both absolute andsigned PEs.

Keywords: anaesthetics i.v., propofol; computer simulation; drug delivery, computerized; pharmacokinetics, models; pharmacokinetics, propofol

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