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氯米帕明、西酞普兰、咪达唑仑及其代谢物在大鼠慢性给药后在骨骼组织中的分布。

Distribution of clomipramine, citalopram, midazolam, and metabolites in skeletal tissue after chronic dosing in rats.

机构信息

Toxicology and Pharmacology, KU Leuven, Leuven, Belgium.

出版信息

Drug Test Anal. 2019 Jul;11(7):1083-1093. doi: 10.1002/dta.2578. Epub 2019 Apr 23.

DOI:10.1002/dta.2578
PMID:30817095
Abstract

In recent years, the use of skeletal tissue as an alternative matrix in forensic toxicology has received new interest. In cases where extreme decomposition has taken place, analysis of skeletal tissue is often the only option left. In this article, a fully validated method is presented and the distribution of clomipramine, citalopram, midazolam, and metabolites after chronically administration is examined within skeletal tissue. Rats were chronically dosed with respectively clomipramine, citalopram, or midazolam. Extracts were quantitatively analyzed using liquid chromatography-electrospray ionization-tandem mass spectrometry (LC-ESI-MS/MS). Clomipramine, citalopram, and metabolites, respectively desmethylclomipramine and desmethylcitalopram are shown to be detectable in all bone types sampled. Midazolam and its metabolite α-OH-midazolam could not be detected. The absence of midazolam in extracts gives an indication that drugs with pKa values under physiological pH are badly or not incorporated in bone tissue. Bone and post-mortem blood concentrations were compared. A range of different bone types was compared and showed that the concentration is strongly dependent on the bone type. In concordance with previous publications, the humerus shows the highest drug levels. Skeletal tissue concentrations found ranged from 1.1 to 587.8 ng/g. Comparison of the same bone type between the different rats showed high variances. However, the drugs-metabolite ratio proved to have lower variances (<20%). Moreover, the drugs-metabolite ratio in the sampled bones is in close concordance to the ratios seen in blood within a rat. From this, we can assume that the drugs-metabolite ratio in skeletal tissue may prove to be more useful than absolute found concentration.

摘要

近年来,骨骼组织作为法医毒理学中替代基质的应用引起了新的关注。在极端分解的情况下,分析骨骼组织通常是唯一的选择。本文提出了一种完全验证的方法,并研究了氯米帕明、西酞普兰、咪达唑仑在慢性给药后在骨骼组织中的分布及其代谢物。大鼠分别给予氯米帕明、西酞普兰或咪达唑仑慢性给药。使用液相色谱-电喷雾电离串联质谱法(LC-ESI-MS/MS)对提取物进行定量分析。在所有采样的骨骼类型中均检测到氯米帕明、西酞普兰及其代谢物分别去甲氯米帕明和去甲西酞普兰。无法检测到咪达唑仑及其代谢物α-OH-咪达唑仑。提取液中未检出咪达唑仑表明,pKa 值低于生理 pH 的药物在骨骼组织中难以或不能被吸收。比较了骨骼和死后血液中的浓度。比较了不同类型的骨骼,结果表明浓度强烈依赖于骨骼类型。与之前的出版物一致,肱骨显示出最高的药物水平。在骨骼组织中发现的浓度范围为 1.1 至 587.8ng/g。不同大鼠的同种骨骼之间的比较显示出很高的差异。然而,药物-代谢物比值的差异较小(<20%)。此外,在采样骨骼中观察到的药物-代谢物比值与大鼠血液中的比值密切一致。由此,我们可以假设骨骼组织中的药物-代谢物比值可能比发现的绝对浓度更有用。

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