Nlmixr2 Versus NONMEM: An Evaluation of Maximum A Posteriori Bayesian Estimates Following External Evaluation of Gentamicin and Tobramycin Population Pharmacokinetic Models

IF 1.5 4区 医学 Q3 PHARMACOLOGY & PHARMACY Clinical Pharmacology in Drug Development Pub Date : 2024-03-11 DOI:10.1002/cpdd.1395
Alexandre Duong, Amélie Marsot
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Abstract

The objective of this project is to compare the results of the same study carried out on NONMEM and nlmixr2. This analysis consists of evaluating previously published population pharmacokinetic models of gentamicin and tobramycin in our population of interest with sparse concentrations. A literature review was performed to determine the gentamicin and tobramycin models in critically ill adult patients. In parallel, gentamicin and tobramycin dosing data, information on the treatment, the patient, and the bacteria were collected retrospectively in 2 Quebec establishments. The external evaluations were previously performed using NONMEM Version 7.5. Model equations were rewritten with R, and external evaluations were performed using nlmixr2. Predictive performance was assessed based on the estimation of bias and imprecision of the prediction error for maximum a posteriori (MAP) Bayesian PK parameter and observed concentrations. Comparison between nlmixr2 and NONMEM was performed on 4 gentamicin and 3 tobramycin population pharmacokinetic models. Compared to NONMEM, for gentamicin and tobramycin clearance and central volume of distribution, nlmixr2 produced individual pharmacokinetic parameters with bias values ranging from −32.5% to 5.67% and imprecision values ranging from 6.33% to 32.5%. Despite these differences, population bias and imprecision for sparse concentrations were low and ranged from 0% to 5.3% and 0.2% to 6.5%, respectively. The external evaluations performed with both software packages resulted in the same interpretation in terms of population predictive performance for all 7 models. Nlmxir2 showed comparable predictive performance with NONMEM with sparse concentrations that are, at most, sampled twice within a single dose administration (peak and trough).

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Nlmixr2 与 NONMEM:外部评估庆大霉素和妥布霉素群体药物动力学模型后的最大后验贝叶斯估计值评估
本项目的目的是比较在 NONMEM 和 nlmixr2 上进行的同一研究的结果。这项分析包括评估以前发表的庆大霉素和妥布霉素在我们感兴趣的人群中的群体药代动力学模型,因为这些人群的浓度稀少。通过文献综述确定了重症成年患者的庆大霉素和妥布霉素模型。与此同时,还在魁北克的两家机构中回顾性地收集了庆大霉素和妥布霉素的剂量数据、治疗信息、患者信息和细菌信息。外部评估之前使用 NONMEM 7.5 版进行。使用 R 重写了模型方程,并使用 nlmixr2 进行了外部评估。预测性能的评估基于对最大后验(MAP)贝叶斯 PK 参数和观测浓度预测误差的偏差和不精确度的估计。对 4 个庆大霉素和 3 个妥布霉素群体药代动力学模型进行了 nlmixr2 与 NONMEM 的比较。就庆大霉素和妥布霉素的清除率和中心分布容积而言,与 NONMEM 相比,nlmixr2 得出的单个药代动力学参数的偏差值在 -32.5% 到 5.67% 之间,不精确值在 6.33% 到 32.5% 之间。尽管存在这些差异,但稀疏浓度的群体偏差和不精确度较低,分别为 0% 至 5.3% 和 0.2% 至 6.5%。使用这两个软件包进行的外部评估对所有 7 个模型的群体预测性能做出了相同的解释。Nlmxir2 与 NONMEM 对稀疏浓度的预测性能相当,稀疏浓度在一次给药中最多采样两次(峰值和谷值)。
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来源期刊
CiteScore
3.70
自引率
10.00%
发文量
154
期刊介绍: Clinical Pharmacology in Drug Development is an international, peer-reviewed, online publication focused on publishing high-quality clinical pharmacology studies in drug development which are primarily (but not exclusively) performed in early development phases in healthy subjects.
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