首页> 外文期刊>Journal of Agricultural and Food Chemistry >Pharmacokinetics of Mequindox and Its Marker Residue 1,4-Bisdesoxymequindox in Swine Following Multiple Oral Gavage and Intramuscular Administration: An Experimental Study Coupled with Population Physiologically Based Pharmacokinetic Modeling
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Pharmacokinetics of Mequindox and Its Marker Residue 1,4-Bisdesoxymequindox in Swine Following Multiple Oral Gavage and Intramuscular Administration: An Experimental Study Coupled with Population Physiologically Based Pharmacokinetic Modeling

机译:多口服饲养和肌肉内给药后梅子吲哚氏素及其标志物残留1,4-双羟基甲基妥索的药代动力学:一种试验研究与种群生理基于药代动力学建模

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摘要

Mequindox (MEQ) is a quinoxaline-N,N-dioxide antibiotic used in food-producing animals. MEQ residue in animal-derived foods is a food safety concern. The tissue distribution of MEQ and its marker residue 1,4-bisdesoxymequindox (Ml) were determined in swine following oral gavage or intramuscular injection twice daily for 3 days. The experimental data were used to construct a flow-limited physiologically based pharmacokinetic (PBPK) model. The model predictions correlated with available data well. Monte Carlo analysis showed that the times needed for Ml concentrations to fall below limit of detection (5 mu g/kg) in liver for the 99th percentile of the population were 27 and 34 days after oral gavage and intramuscular administration twice daily for 3 days, respectively. This population PBPK model can be used to predict depletion kinetic profiles and tissue residues of MEQs marker residue Ml in swine and as a foundation for scaling to other quinoxaline-N,N-dioxide antibiotics and to other animal species.
机译:MEQUINDOX(MEQ)是一种用于食品动物的喹喔啉-N,二氧化二锑抗生素。动物衍生食品中的MEQ残留是一种食品安全问题。 MEQ及其标记物残留物1,4-双氧基yequIndox(ml)的组织分布在口服饲养或肌肉注射后每天两次测定3天。实验数据用于构建流动限制的生理学药代动力学(PBPK)模型。模型预测与可用数据相关的相关性。 Monte Carlo分析表明,ML浓度低于肝脏的浓度低于肝脏(5μg/ kg)的时间为99百分位数,在口服饲养和肌肉内给药后27天,34天,每天3天,分别。该群体PBPK模型可用于预测猪中MEQS标志物残留物M1的耗尽动力学曲线和组织残留物,作为缩放到其他喹喔啉-N,二氧化氮抗生素和其他动物物种的基础。

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