作者
Kenichi Masui, Richard N Upton, Anthony G Doufas, Johan F Coetzee, Tomiei Kazama, Eric P Mortier, Michel MRF Struys
发表日期
2010/1/1
期刊
Anesthesia and Analgesia
卷号
111
期号
2
简介
BACKGROUND:
With the growing use of pharmacokinetic (PK)-driven drug delivery and/or drug advisory displays, identifying the PK model that best characterizes propofol plasma concentration (Cp) across a variety of dosing conditions would be useful. We tested the accuracy of 3 compartmental models and 1 physiologically based recirculatory PK model for propofol to predict the time course of propofol Cp using concentration-time data originated from studies that used different infusion schemes.
METHODS:
Three compartmental PK models for propofol, called the “Marsh,” the “Schnider,” and the “Schüttler” models, and 1 physiologically based recirculatory model called the “Upton” model, were used to simulate the time course of propofol Cp. To test the accuracy of the models, we used published measured plasma concentration data that originated from studies of manual (bolus and short infusion) and computer …
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