首页> 美国卫生研究院文献>CPT: Pharmacometrics Systems Pharmacology >Modeling of Large Pharmacokinetic Data Using Nonlinear Mixed‐Effects: A Paradigm Shift in Veterinary Pharmacology. A Case Study With Robenacoxib in Cats
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Modeling of Large Pharmacokinetic Data Using Nonlinear Mixed‐Effects: A Paradigm Shift in Veterinary Pharmacology. A Case Study With Robenacoxib in Cats

机译:使用非线性混合效应对大型药代动力学数据进行建模:兽医药理学的范式转变。罗贝奈昔在猫中的案例研究

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摘要

The objective of this study was to model the pharmacokinetics (PKs) of robenacoxib in cats using a nonlinear mixed‐effects (NLME) approach, leveraging all available information collected from cats receiving robenacoxib s.c. and/or i.v.: 47 densely sampled laboratory cats and 36 clinical cats sparsely sampled preoperatively. Data from both routes were modeled sequentially using Monolix 4.3.2. Influence of parameter correlations and available covariates (age, gender, bodyweight, and anesthesia) on population parameter estimates were evaluated by using multiple samples from the posterior distribution of the random effects. A bicompartmental disposition model with simultaneous zero and first‐order absorption best described robenacoxib PKs in blood. Clearance was 0.502 L/kg/h and the bioavailability was high (78%). The absorption constant point estimate (Ka = 0.68 h−1) was lower than beta (median, 1.08 h−1), unveiling flip‐flop kinetics. No dosing adjustment based on available covariates information is advocated. This modeling work constitutes the first application of NLME in a large feline population.
机译:这项研究的目的是利用非线性混合效应(NLME)方法对罗贝纳昔布在猫中的药代动力学(PKs)进行建模,并利用从接受罗贝纳昔布s.c的猫中收集的所有可用信息。和/或i.v .:术前稀疏采样的47只实验室猫和36只临床猫。使用Monolix 4.3.2对来自两条路径的数据进行顺序建模。通过使用随机效应的后验分布中的多个样本,评估了参数相关性和可用的协变量(年龄,性别,体重和麻醉)对人群参数估计值的影响。具有零和一阶同时吸收的双室处置模型最能描述血液中的罗贝纳昔PK。清除率为0.502 L / kg / h,生物利用度较高(78%)。吸收常数估算值(Ka = 0.68 h -1 )低于beta(中位数,1.08 h -1 ),揭示了触发器动力学。不主张基于可用的协变量信息进行剂量调整。这项建模工作构成了NLME在大量猫科动物中的首次应用。

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