群体药代动力学减少估算新生儿动力学参数所需的血液采样频率的潜力。

L. Collart, T. Blaschke, F. Boucher, C. Prober
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引用次数: 33

摘要

从接受齐多夫定的新生儿中获得的数据作为I期研究的一部分,用于估计该药物的总体药代动力学参数,并确定提供准确估计动力学参数及其变异性所需的最小数据点数。采用非线性混合效应模型(NONMEM)对32名婴儿的541个齐多夫定浓度进行了分析。减少的数据集是通过随机减少每个给药间隔的抽样时间点数量和/或随机减少可用受试者的数量而得到的。我们确定了准确估计药代动力学参数及其变异性,包括所有32例患者,每个剂量间隔仅使用两个浓度时间点,前提是其中一个时间点是在给药后的前2小时内获得的。仅用24名受试者和每个剂量间隔的两个浓度时间点即可充分估计参数本身。我们建议,除了传统的药代动力学分析外,还应使用NONMEM,以最少的每位患者血液采样,直接在感兴趣的人群中获得更精确的信息。这对血容量有限的婴儿尤其重要。
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Potential of population pharmacokinetics to reduce the frequency of blood sampling required for estimating kinetic parameters in neonates.
Data obtained from neonates receiving zidovudine as part of a phase I study were used to estimate the population pharmacokinetic parameters of this drug and to determine the minimum number of data points necessary to provide accurate estimates of the kinetic parameters and their variability. Analysis was performed with 541 concentrations of zidovudine, obtained from 32 infants and with a variety of reduced data sets using NONMEM (nonlinear mixed effect model). The reduced data sets were derived by randomly reducing the number of sampling time points per dosing interval and/or by randomly reducing the number of available subjects. We determined that accurate estimates of pharmacokinetic parameters and their variability were obtained with the inclusion of all 32 patients using only two concentration-time points per dose interval, provided that one of the points was obtained during the first 2 h after administration of the drug. The parameters themselves were adequately estimated with only 24 subjects and two concentration-time points per dose interval. We suggest that NONMEM should be used in addition to the traditional pharmacokinetic analysis to obtain more precise information directly in the population of interest with a minimum of blood sampling from each patient. This is especially critical in infants whose blood volumes are limited.
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