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口服布地奈德后在人尿中代谢物的鉴定。

Identification of budesonide metabolites in human urine after oral administration.

机构信息

Bioanalysis Research Group, IMIM, Institut de Recerca Hospital del Mar, Doctor Aiguader 88, 08003, Barcelona, Spain.

出版信息

Anal Bioanal Chem. 2012 Aug;404(2):325-40. doi: 10.1007/s00216-012-6037-0. Epub 2012 May 10.

DOI:10.1007/s00216-012-6037-0
PMID:22573060
Abstract

Budesonide (BUD) is a glucocorticoid widely used for the treatment of asthma, rhinitis, and inflammatory bowel disease. Its use in sport competitions is prohibited when administered by oral, intravenous, intramuscular, or rectal routes. However, topical preparations are not prohibited. Strategies to discriminate between legal and forbidden administrations have to be developed by doping control laboratories. For this reason, metabolism of BUD has been re-evaluated using liquid chromatography-tandem mass spectrometry (LC-MS/MS) with different scan methods. Urine samples obtained after oral administration of 3 mg of BUD to two healthy volunteers have been analyzed for metabolite detection in free and glucuronide metabolic fractions. Structures of the metabolites have been studied by LC-MS/MS using collision induced dissociation and gas chromatography-mass spectrometry (GC/MS) in full scan mode with electron ionization. Combination of all structural information allowed the proposition of the most comprehensive picture for BUD metabolism in humans to this date. Overall, 16 metabolites including ten previously unreported compounds have been detected. The main metabolite is 16α-hydroxy-prednisolone resulting from the cleavage of the acetal group. Other metabolites without the acetal group have been identified such as those resulting from reduction of C20 carbonyl group, oxidation of the C11 hydroxyl group and reduction of the A ring. Metabolites maintaining the acetal group have also been identified, resulting from 6-hydroxylation (6α and 6β-hydroxy-budesonide), 23-hydroxylation, reduction of C6-C7, oxidation of the C11 hydroxyl group, and reduction of the C20 carbonyl group. Metabolites were mainly excreted in the free fraction. All of them were excreted in urine during the first 24 h after administration, and seven of them were still detected up to 48 h after administration for both volunteers.

摘要

布地奈德(BUD)是一种广泛用于治疗哮喘、鼻炎和炎症性肠病的糖皮质激素。当通过口服、静脉、肌肉或直肠途径给药时,其在体育比赛中的使用是被禁止的。然而,局部制剂不受禁止。兴奋剂控制实验室必须制定策略来区分合法和禁止的给药。出于这个原因,使用不同的扫描方法,使用液相色谱-串联质谱(LC-MS/MS)重新评估了 BUD 的代谢。对两名健康志愿者口服 3mg BUD 后的尿液样品进行了分析,以检测游离和葡萄糖醛酸代谢物分数中的代谢物。使用 LC-MS/MS 结合碰撞诱导解离和气相色谱-质谱(GC/MS)在全扫描模式下进行电子电离,研究了代谢物的结构。所有结构信息的结合使得迄今为止能够对 BUD 在人体内的代谢提出最全面的描述。总的来说,已经检测到包括十种以前未报道的化合物在内的 16 种代谢物。主要代谢物是 16α-羟基泼尼松龙,这是乙缩醛基团裂解的结果。还鉴定了其他没有乙缩醛基团的代谢物,例如 C20 羰基还原、C11 羟基氧化和 A 环还原的产物。还鉴定了保持乙缩醛基团的代谢物,它们来自 6-羟基化(6α 和 6β-羟基布地奈德)、23-羟基化、C6-C7 还原、C11 羟基氧化和 C20 羰基还原。代谢物主要以游离形式排泄。两者志愿者在给药后 24 小时内尿液中均排泄了所有代谢物,并且在给药后 48 小时仍检测到其中七种代谢物。

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