首页> 美国卫生研究院文献>CPT: Pharmacometrics Systems Pharmacology >From Pediatric Covariate Model to Semiphysiological Function for Maturation: Part I–Extrapolation of a Covariate Model From Morphine to Zidovudine
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From Pediatric Covariate Model to Semiphysiological Function for Maturation: Part I–Extrapolation of a Covariate Model From Morphine to Zidovudine

机译:从儿童协变量模型到成熟的半生理功能:第一部分–吗啡到齐多夫定协变量模型的外推

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摘要

New approaches to expedite the development of safe and effective pediatric dosing regimens and first-in-child doses are urgently needed. Model-based approaches require quantitative functions on the maturation of different metabolic pathways. In this study, we directly incorporated a pediatric covariate model for the glucuronidation of morphine into a pediatric population model for zidovudine glucuronidation. This model was compared with a reference model that gave the statistically best description of the data. Both models had adequate goodness-of-fit plots and normalized prediction distribution errors (NPDE), similar population clearance values for each individual, and a Δobjective function value of 13 points (Δ2df). This supports our hypothesis that pediatric pharmacokinetic covariate models contain system-specific information that can be used as semiphysiological functions in pediatric population models. Further research should explore the validity of the semiphysiological function for other UDP-glucuronosyltransferase 2B7 substrates and patient populations and reveal how this function can be used for pediatric physiologically based pharmacokinetic models.
机译:迫切需要新的方法来加快安全有效的儿科给药方案和婴儿剂量的发展。基于模型的方法需要对不同代谢途径的成熟进行定量分析。在这项研究中,我们将吗啡葡萄糖醛酸化的儿科协变量模型直接纳入齐多夫定葡萄糖醛酸化的儿科人群模型中。该模型与参考模型进行了比较,该模型给出了数据的统计学上最好的描述。两种模型均具有足够的拟合优度图和归一化的预测分布误差(NPDE),每个个体的相似总体清除值,以及13个点的Δ目标函数值(Δ2df)。这支持了我们的假设,即小儿药代动力学协变量模型包含特定于系统的信息,这些信息可用作小儿群体模型的半生理功能。进一步的研究应探索其他UDP-葡萄糖醛酸转移酶2B7底物和患者群体的半生理功能的有效性,并揭示该功能如何用于儿科基于生理学的药代动力学模型。

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