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Bayesian evaluation of a physiologically-based pharmacokinetic (PBPK) model of long-term kinetics of metal nanoparticles in rats

机译:贝叶斯模型评估大鼠金属纳米颗粒长期动力学的基于生理的药代动力学(PBPK)模型

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摘要

Biomathematical modeling quantitatively describes the disposition of metal nanoparticles in lungs and other organs of rats. In a preliminary model, adjustable parameters were calibrated to each of three data sets using a deterministic approach, with optimal values varying among the different data sets. In the current effort, Bayesian population analysis using Markov chain Monte Carlo (MCMC) simulation was used to recalibrate the model while improving assessments of parameter variability and uncertainty. The previously-developed model structure and some physiological parameter values were modified to improve physiological realism. The data from one of the three previously-identified studies and from two other studies were used for model calibration. The data from the one study that adequately characterized mass balance were used to generate parameter distributions. When data from a second study of the same nanomaterial (iridium) were added, the level of agreement was still acceptable. Addition of another data set (for silver nanoparticles) led to substantially lower precision in parameter estimates and large discrepancies between the model predictions and experimental data for silver nanoparticles. Additional toxicokinetic data are needed to further evaluate the model structure and performance and to reduce uncertainty in the kinetic processes governing in vivo disposition of metal nanoparticles.
机译:生物数学模型定量描述了金属纳米颗粒在大鼠肺和其他器官中的分布。在初步模型中,使用确定性方法将可调参数校准到三个数据集中的每个,最佳值在不同数据集之间变化。在当前的工作中,使用马尔可夫链蒙特卡洛(MCMC)模拟进行的贝叶斯人口分析被用于重新校准模型,同时改善了对参数变异性和不确定性的评估。修改了先前开发的模型结构和一些生理参数值,以改善生理真实感。来自三个先前确定的研究之一和来自其他两个研究的数据用于模型校准。一项研究的数据充分表征了质量平衡,用于生成参数分布。当添加来自同一纳米材料(铱)的第二项研究的数据时,一致性水平仍然可以接受。添加另一个数据集(用于银纳米颗粒)导致参数估计的精度大大降低,并且模型预测与银纳米颗粒的实验数据之间存在较大差异。需要更多的毒代动力学数据来进一步评估模型的结构和性能,并减少控制金属纳米粒子体内处置的动力学过程的不确定性。

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