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首页> 外文期刊>Journal of applied toxicology >Calibration and validation of a physiologically based model for soman intoxication in the rat, marmoset, guinea pig and pig
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Calibration and validation of a physiologically based model for soman intoxication in the rat, marmoset, guinea pig and pig

机译:基于生理学模型的大鼠,mar猴,豚鼠和猪的梭曼中毒模型的校准和验证

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摘要

A physiologically based pharmacokinetic and pharmacodynamic (PBPK/PD) model has been developed for low, medium and high levels of soman intoxication in the rat, marmoset, guinea pig and pig. The primary objective of this model was to describe the pharmacokinetics of soman after intravenous, intramuscular and subcutaneous administration in the rat, marmoset, guinea pig, and pig as well as its subsequent pharmacodynamic effects on blood acetylcholinesterase (AChE) levels, relating dosimetry to physiological response. The reactions modelled in each physiologically realistic compartment are: (1) partitioning of C(±)P(±) soman from the blood into the tissue; (2) inhibition of AChE and carboxylesterase (CaE) by soman; (3) elimination of soman by enzymatic hydrolysis; (4) de novo synthesis and degradation of AChE and CaE; and (5) aging of AChE-soman and CaE-soman complexes. The model was first calibrated for the rat, then extrapolated for validation in the marmoset, guinea pig and pig. Adequate fits to experimental data on the time course of soman pharmacokinetics and AChE inhibition were achieved in the mammalian models. In conclusion, the present model adequately predicts the dose-response relationship resulting from soman intoxication and can potentially be applied to predict soman pharmacokinetics and pharmacodynamics in other species, including human.
机译:已开发出一种基于生理学的药代动力学和药效学(PBPK / PD)模型,用于大鼠,mar猴,豚鼠和猪中梭曼中毒的低,中和高水平。该模型的主要目的是描述大鼠、,猴,豚鼠和猪静脉内,肌肉内和皮下给药后梭曼的药代动力学,以及其随后对血液乙酰胆碱酯酶(AChE)水平的药效作用,并将剂量学与生理学相关响应。在每个生理现实区室中建模的反应是:(1)将C(±)P(±)梭曼从血液分配到组织中; (2)梭曼对AChE和羧酸酯酶(CaE)的抑制作用; (3)通过酶水解消除梭曼; (4)从头合成和降解AChE和CaE; (5)AChE-梭曼和CaE-梭曼复合物的老化。首先针对大鼠对模型进行校准,然后外推以在mo猴,豚鼠和猪中进行验证。在哺乳动物模型中获得了关于梭曼药代动力学和AChE抑制时间过程的实验数据的充分拟合。总之,本模型充分预测了梭曼中毒引起的剂量反应关系,并且可以潜在地用于预测梭曼在其他物种(包括人类)中的药代动力学和药效学。

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