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多重非靶向框架能够通过气相色谱-轨道阱-高分辨质谱在纳克水平追踪氧甲氢龙和美睾酮的体内代谢谱,用于反兴奋剂目的。

Multiplex Nontargeted Framework Enables Tracking Metabolic Profile of Oxymetholone and Methasterone In Vivo at Nanogram Level by GC-Orbitrap-HRMS for Antidoping Purpose.

作者信息

Zheng Siying, Ge Yuqi, Fang Xian, Liu Mengpan, Sun Haoyi, Deng Xiaojun, Liao Lei

机构信息

Shanghai University of Sport, 399 Changhai Road, Shanghai 200438, China.

Shanghai Anti-doping Laboratory, 900 Jiangwancheng Road, Shanghai 200438, China.

出版信息

Anal Chem. 2025 Feb 11;97(5):3009-3018. doi: 10.1021/acs.analchem.4c06026. Epub 2025 Jan 30.

Abstract

Oxymetholone and methasterone are anabolic androgenic steroids prohibited by the World Anti-Doping Agency (WADA) for both in-competition and out-of-competition use. Detecting metabolites of exogenous steroids is crucial for establishing doping violations, making the study of these metabolites essential in antidoping efforts. This study investigated the urinary metabolic profiles of oxymetholone and methasterone using gas chromatography-orbitrap high-resolution mass spectrometry (GC-Orbitrap-HRMS) in nanogram level by utilizing a novel multiplex nontargeted framework protocol. Healthy volunteers each ingested one tablet of the drug, and urine samples were collected over 50 days in postadministration phase. The complete detection of the three fractions (free fraction, glucuronide fraction, and sulfate fraction) of the metabolites was carried out. The GC-Orbitrap-HRMS full-scan mode was employed to detect postadministration urine samples, comparing these with preadministration baseline urine samples to identify newly formed substances. Electron ionization (EI) mass spectra were used to infer possible metabolite structures, leading to the discovery of three novel metabolites of oxymetholone and two novel metabolites of methasterone. Notably, the newly identified oxymetholone metabolite, 2-methylene-17α-methyl-androstane-16ξ,17β-diol-3-one (O-M6), was detectable as a glucuronide conjugate up to 4 days after administration. The methasterone metabolite, 18-nor-17β-hydroxymethyl-2α,17α-dimethyl-5α-androst-13-en-3-one (M-M4), exhibited prolonged detectability as a glucuronide conjugate, being present in urine samples from both volunteers up to 50 days after administration. These findings have significant implications for antidoping purpose, providing extended detection windows for these anabolic steroids.

摘要

氧甲氢龙和美睾酮是世界反兴奋剂机构(WADA)禁止在比赛中和比赛外使用的合成代谢雄激素类固醇。检测外源性类固醇的代谢产物对于确定兴奋剂违规行为至关重要,因此对这些代谢产物的研究在反兴奋剂工作中必不可少。本研究采用一种新型的多重非靶向框架方案,利用气相色谱 - 轨道阱高分辨率质谱(GC-Orbitrap-HRMS)在纳克水平上研究了氧甲氢龙和美睾酮的尿液代谢谱。健康志愿者每人服用一片药物,并在给药后的50天内收集尿液样本。对代谢产物的三个部分(游离部分、葡萄糖醛酸苷部分和硫酸盐部分)进行了全面检测。采用GC-Orbitrap-HRMS全扫描模式检测给药后的尿液样本,并将其与给药前的基线尿液样本进行比较,以识别新形成的物质。利用电子电离(EI)质谱推断可能的代谢产物结构,从而发现了氧甲氢龙的三种新型代谢产物和美睾酮的两种新型代谢产物。值得注意的是,新鉴定出的氧甲氢龙代谢产物2-亚甲基-17α-甲基-雄甾烷-16ξ,17β-二醇-3-酮(O-M6)在给药后4天内可作为葡萄糖醛酸苷共轭物被检测到。美睾酮代谢产物18-去甲-17β-羟甲基-2α,17α-二甲基-5α-雄甾-13-烯-3-酮(M-M4)作为葡萄糖醛酸苷共轭物的可检测时间延长,在两名志愿者的尿液样本中给药后50天仍存在。这些发现对反兴奋剂目的具有重要意义,为这些合成代谢类固醇提供了更长的检测窗口期。

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