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在 3 名志愿者中经口服和皮肤给药后二正丁基己二酸(DnBA)的人体代谢和尿排泄动力学。

Human metabolism and urinary excretion kinetics of di-n-butyl adipate (DnBA) after oral and dermal administration in three volunteers.

机构信息

Institute for Prevention and Occupational Medicine of the German Social Accident Insurance, Institute of the Ruhr-University Bochum (IPA), Bürkle-de-la-Camp-Platz 1, 44789, Bochum, Germany.

Institute for Prevention and Occupational Medicine of the German Social Accident Insurance, Institute of the Ruhr-University Bochum (IPA), Bürkle-de-la-Camp-Platz 1, 44789, Bochum, Germany.

出版信息

Toxicol Lett. 2021 Jun 1;343:11-20. doi: 10.1016/j.toxlet.2021.02.012. Epub 2021 Feb 25.

Abstract

Di-n-butyl adipate (DnBA) is used as a plasticizer and in various consumer products (e.g. personal care products) replacing, in part, the endocrine disruptor di-n-butyl phthalate (DnBP). We provide quantitative in vivo data on human DnBA metabolism and excretion after oral dose (105-185 μg/kg bw) and dermal application to three volunteers each as a tool for exposure and risk assessment. Complete and consecutive urine samples were collected for two (oral) and four days (dermal), respectively, and analyzed for the metabolites mono-n-butyl adipate (MnBA), 3- and tentative 4-hydroxy-mono-n-butyl adipate (3OH-MnBA, 4OH-MnBA), and 3-carboxy-mono-n-propyl adipate (3cx-MnPrA), as well as the hydrolysis product adipic acid (AA) using stable isotope dilution quantification. Metabolites were excreted within 24 h after oral dose with one or two concentration maxima at 0.8-3.0 h (n = 3) and 4.8-6.3 h (n = 2). AA was the major but unspecific metabolite with urinary excretion fractions (Fs) of 14-26 %. Mean Fs (range) of 3cx-MnPrA, MnBA, 3OH-MnBA, and tentative 4OH-MnBA were low, but consistent between volunteers (0.47 % (0.35-0.63 %), 0.079 % (0.065-0.091 %), 0.012 % (0.006-0.016 %), and 0.005 % (0.002-0.009 %), respectively). MnBA and 3OH-MnBA seem to be suitable, specific exposure biomarkers for DnBA, whereas 3cx-MnPrA and 4OH-MnBA seem to originate also from other, unknown sources not related to DnBA. Compared to the oral study, metabolite excretion in the dermal study was delayed and MnBA excretion was somewhat higher compared to the oxidized metabolites. Based on urinary concentrations and the above excretion fractions, calculated uptakes in the dermal study did not exceed the adipate ester ADI of 5 mg/(kg bw*day).

摘要

己二酸二正丁酯(DnBA)用作增塑剂,用于各种消费品(例如个人护理产品),部分替代内分泌干扰物邻苯二甲酸二正丁酯(DnBP)。我们提供了志愿者口服(105-185μg/kg bw)和经皮应用后体内 DnBA 代谢和排泄的定量数据,作为暴露和风险评估的工具。分别连续收集完整的尿液样本 2 天(口服)和 4 天(经皮),并使用稳定同位素稀释定量法分析代谢物单正丁基己二酸(MnBA)、3-和暂定 4-羟基单正丁基己二酸(3OH-MnBA)、3-羧基单正丙基己二酸(3cx-MnPrA)以及水解产物己二酸(AA)。口服剂量后 24 小时内排泄代谢物,在 0.8-3.0 h(n = 3)和 4.8-6.3 h(n = 2)时出现一个或两个浓度峰值。AA 是主要但非特异性的代谢物,尿排泄分数(Fs)为 14-26%。3cx-MnPrA、MnBA、3OH-MnBA 和暂定 4OH-MnBA 的平均 Fs(范围)较低,但志愿者之间一致(0.47%(0.35-0.63%)、0.079%(0.065-0.091%)、0.012%(0.006-0.016%)和 0.005%(0.002-0.009%))。MnBA 和 3OH-MnBA 似乎是 DnBA 的合适、特异性暴露生物标志物,而 3cx-MnPrA 和 4OH-MnBA 似乎也来自其他与 DnBA 无关的未知来源。与口服研究相比,经皮研究中的代谢物排泄延迟,MnBA 排泄量与氧化代谢物相比略高。基于尿液浓度和上述排泄分数,经皮研究中的摄入量计算未超过己二酸酯 ADI(5mg/(kg bw*day))。

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