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Update on a Pharmacokinetic-Centric Alternative Tier II Program for MMT—Part II: Physiologically Based Pharmacokinetic Modeling and Manganese Risk Assessment

机译:MMT的药代动力学中心替代方法II更新-第二部分:基于生理的药代动力学模型和锰风险评估

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摘要

Recently, a variety of physiologically based pharmacokinetic (PBPK) models have been developed for the essential element manganese. This paper reviews the development of PBPK models (e.g., adult, pregnant, lactating, and neonatal rats, nonhuman primates, and adult, pregnant, lactating, and neonatal humans) and relevant risk assessment applications. Each PBPK model incorporates critical features including dose-dependent saturable tissue capacities and asymmetrical diffusional flux of manganese into brain and other tissues. Varied influx and efflux diffusion rate and binding constants for different brain regions account for the differential increases in regional brain manganese concentrations observed experimentally. We also present novel PBPK simulations to predict manganese tissue concentrations in fetal, neonatal, pregnant, or aged individuals, as well as individuals with liver disease or chronic manganese inhalation. The results of these simulations could help guide risk assessors in the application of uncertainty factors as they establish exposure guidelines for the general public or workers.
机译:最近,针对必需元素锰开发了多种基于生理学的药代动力学(PBPK)模型。本文回顾了PBPK模型(例如成年,怀孕,哺乳和新生大鼠,非人类灵长类动物以及成年,怀孕,哺乳和新生人类)的发展以及相关的风险评估应用。每个PBPK模型都包含一些关键特征,包括剂量依赖性的饱和组织容量以及锰进入大脑和其他组织的不对称扩散通量。不同脑区域的各种流入量和外排扩散率以及结合常数说明了实验观察到的区域性脑锰浓度的差异性增加。我们还提出了新颖的PBPK模拟,以预测胎儿,新生儿,孕妇或老年个体以及患有肝病或慢性锰吸入的个体中的锰组织浓度。这些模拟的结果可帮助指导风险评估师建立不确定性因素,从而为一般公众或工人制定暴露准则。

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