人类PBBK模型的发展混合物:汞,铅和硒的三重奏混合物

D. D. Maza, J. Ojo
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引用次数: 2

摘要

建立了一种基于生理的生物动力学(PBBK)模型,用于同时预测铅、汞和硒在人体许多靶组织中的ADME特性。我们在以前的研究中开发的汞、铅和硒的独立模型被整合到这些元素混合物的单一模型中。口服剂量单位为μmol/kg/d,组织浓度单位为μmol/kg。这种整合是基于这样一个事实,即这些元素之间的相互作用会影响它们在各自组织中的生物积累,从而导致它们的分配系数的改变。汞和铅的联合口服剂量分为低剂量或高剂量,而硒的剂量分为低剂量、适当剂量或高剂量。汞铅联合剂量为低剂量,硒剂量也为低剂量,肝、肾、脑、充分灌注组织和缓慢灌注组织中汞和铅的浓度分别受2.01、0.91、1.5、0.91和0.90因子的调节,硒的浓度分别受0.03、0.21、0.89、0.75和0.75因子的调节。另一方面,在汞铅联合剂量为高、硒联合剂量为低的情况下,汞和铅的浓度分别受1.51、0.68、1.28、1.45和1.45因子的调节,硒的浓度分别受0.05、0.30、0.45、0.60和0.60因子的调节。在硒摄入量充足、汞铅联合剂量为高的情况下,各组织中汞和铅的浓度不受调节,而肝、肾、脑、充分灌注组织和缓慢灌注组织中硒的浓度分别受0.82、2.89、0.96、0.64和0.64因子的调节。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Development of a Human PBBK Model for Mixtures: Trio Mixture of Mercury, Lead, and Selenium
A physiologically-based biokinetic (PBBK) model has been developed for predicting simultaneously the ADME properties of lead, mercury, and selenium in a number of target tissues of humans. Independent models for mercury, lead and selenium which were developed in a previous study undertaken by us were integrated into a single model for the mixture of these elements. Oral doses were presented in μmol/kg/day, while tissue concentrations were in μmol/kg. The integration was based on the fact that interaction among these elements affects their bioaccumulation in the respective tissues, resulting in alterations to their partition coefficients. Combined oral doses of mercury and lead were categorized as either low or high, while selenium doses were categorized as either low, adequate or high. With the combined dose of mercury and lead categorized as low, and selenium dose also categorized as low, the concentration of mercury and lead in the liver, kidney, brain, richly perfused tissues, and slowly perfused tissues were modulated by factors of 2.01, 0.91, 1.5, 0.91, and 0.90, respectively, while the concentration of selenium in these tissues were modulated by factors of 0.03, 0.21, 0.89, 0.75, and 0.75, respectively. On the other hand, with the combined dose of mercury and lead categorized as high and selenium dose categorized as low, the concentration of mercury and lead in these tissues were modulated by factors of 1.51, 0.68, 1.28, 1.45, and 1.45, respectively, while that of selenium were modified by factors of 0.05, 0.30, 0.45, 0.60, and 0.60, respectively. With adequate selenium intake and combined dose of mercury and lead categorized as high, the concentration of mercury and lead in the various tissues were not modulated, while the concentration of selenium in the liver, kidney, brain, richly perfused tissues, and slowly perfused tissues were modulated by factors of 0.82, 2.89, 0.96, 0.64, and 0.64, respectively.
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