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首页> 外文期刊>Talanta: The International Journal of Pure and Applied Analytical Chemistry >Simultaneous determination of phenoxyethanol and its major metabolite, phenoxyacetic acid, in rat biological matrices by LC-MS/MS with polarity switching: Application to ADME studies
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Simultaneous determination of phenoxyethanol and its major metabolite, phenoxyacetic acid, in rat biological matrices by LC-MS/MS with polarity switching: Application to ADME studies

机译:极性切换LC-MS / MS同时测定大鼠生物基质中苯氧乙醇及其主要代谢产物苯氧乙酸:在ADME研究中的应用

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摘要

This study describes the development of a simple LC-ESI-MS/MS method with polarity switching for the simultaneous analysis of phenoxyethanol (PE) and its major metabolite, phenoxyacetic acid (PAA), in rat plasma, urine, and 7 different tissues. The assay was validated to demonstrate the linearity, precision, accuracy, LLOQ recovery, and stability by using the matrix matched QC samples. The assay achieved the LLOQ of 10 and 20 ng/mL of PE and PAA, respectively, for plasma samples and the LLOQ of 20 and 50 ng/mL of PE and PAA, respectively, for urine and tissue samples. This method was successfully applied to the percutaneous absorption, distribution, metabolism, and excretion studies in rats. The absolute topical bioavailability of PE was 75.4% and 76.0% for emulsion and lotion, respectively. Conversion of PE to PAA was extensive, with the average AUC(PAA)-to-AUC(PE) ratio being 4.4 and 5.3 for emulsion and lotion, respectively. The steady-state tissue-to-plasma PE concentration ratio (K-p) was higher than unity for kidney, spleen, heart, brain, and testis and was lower (<= 0.6) for lung and liver, while the metabolite ratio was higher than unity for kidney, liver, lung, and testis and was lower (<= 0.3) for other tissues. Findings of this study may be useful to evaluate the relationship between exposure and toxic potential of PE in risk assessment. (C) 2015 Elsevier B.V. All rights reserved.
机译:这项研究描述了一种简单的具有极性切换功能的LC-ESI-MS / MS方法的开发,用于同时分析大鼠血浆,尿液和7种不同组织中的苯氧基乙醇(PE)及其主要代谢产物苯氧基乙酸(PAA)。通过使用基质匹配的QC样品验证了该测定方法的线性,精密度,准确性,LLOQ回收率和稳定性。该测定对血浆样品的PE和PAA的LLOQ分别为10和20 ng / mL,对尿液和组织样品的PE和PAA的LLOQ分别为20和50 ng / mL。该方法已成功应用于大鼠的经皮吸收,分布,代谢和排泄研究。乳液和乳液的PE绝对局部生物利用度分别为75.4%和76.0%。 PE到PAA的转化非常广泛,乳液和乳液的平均AUC(PAA)/ AUC(PE)比分别为4.4和5.3。肾脏,脾脏,心脏,大脑和睾丸的稳态组织血浆血浆PE浓度比(Kp)高于单位,而肺和肝脏的稳态组织血浆血浆PE浓度比(Kp)低于(<= 0.6),而代谢物比率高于肾,肝,肺和睾丸的单位统一,其他组织则较低(<= 0.3)。这项研究的结果可能有助于评估风险评估中PE的暴露与潜在毒性之间的关系。 (C)2015 Elsevier B.V.保留所有权利。

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