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Individualising gentamicin dosage regimens. A comparative review of selected models, data fitting methods and monitoring strategies.

作者信息

Jelliffe R W, Iglesias T, Hurst A K, Foo K A, Rodriguez J

机构信息

Laboratory of Applied Pharmacokinetics, University of Southern California, School of Medicine, Los Angeles.

出版信息

Clin Pharmacokinet. 1991 Dec;21(6):461-78. doi: 10.2165/00003088-199121060-00006.

DOI:10.2165/00003088-199121060-00006
PMID:1782740
Abstract

The various components required for individualising clinical drug dosage regimens are reviewed, including a study of 3 types of fitting procedures, 2 types of gentamicin pharmacokinetic model and the utility of D-optimal times for obtaining serum gentamicin concentrations. The combination of the current Bayesian fitting procedure, the kslope pharmacokinetic model [in which the elimination rate constant (kel) can change from dose to dose with changing creatinine clearance] and the explicit measurement of the assay error pattern yielded predictions of future serum gentamicin concentrations which were (a) slightly better than those found using weighted nonlinear least squares; (b) somewhat better than those found with Bayesian fitting and a fixed-kel model; (c) better than those found using the traditional linear regression fitting procedure and a fixed kel model. D-Optimally timed pairs of concentrations also predicted future concentrations at least as well, and more cost effectively.

摘要

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