用于兴奋剂控制应用的骆驼尿液中皮质类固醇、小肽、SARM 和季铵类药物的同步检测方法开发与验证

IF 1.7 4区化学 Q3 CHEMISTRY, ANALYTICAL

Current Analytical Chemistry Pub Date : 2024-01-08 DOI:10.2174/0115734110276595231222050709

Jahfar Nalakath, Rasik PT, Praseen OK, Shamil P, N Selvapalam, ER Nagarajan

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引用次数: 0

摘要

背景：对包括小肽、皮质类固醇、选择性雄激素受体调节剂（SARMs）和季铵盐类药物（QADs）在内的多种药物进行检测和鉴定是多个领域的当务之急，特别是在反兴奋剂分析中，鉴于这些药物可能在动物运动中被滥用，因此迫切需要一种全面的筛查方法来有效鉴定这些化合物。目标：开发一种稳健灵敏的高分辨率方法，利用液相色谱精确质谱法同时筛查赛后尿样中的小肽、皮质类固醇、SARMs 和 QADs。该方法整合了简化的单级萃取方法，大大提高了筛查各类药物的效率和适应性。方法：该方法的开发和验证涉及一个全面的固相萃取方案，包括皮质类固醇、小肽、SARMs 和 QADs 的顺序洗脱。使用反相 C18 色谱柱实现色谱分离，并使用液相色谱-高分辨精确质谱法进行分析。结果：所开发的方法通过了各类药物的验证。该方法表现出稳健性和灵敏度，可同时筛选指定类别的药物。所建议的提取和分析方法具有灵活性，可无缝整合新的候选药物，无需重新开发方法。结论成功开发并验证了一种多功能、有效的筛选方法，可同时检测小肽、皮质类固醇、SARMs 和 QADs。该方法能够利用全扫描 HRMS 对新出现的药物进行回顾性分析，从而提高了其实用性。该方法在必须进行准确、全面药物筛选的各个领域大有可为。

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Method Development and Validation for Simultaneous Detection of Corticosteroids, Small Peptides, SARMs and Quaternary Ammonium Drugs in Camel Urine for Doping Control Applications

Background: Detection and identification of a wide range of drugs, including small peptides, corticosteroids, selective androgen receptor modulators (SARMs), and quaternary ammonium drugs (QADs), are imperative across several domains, particularly in anti-doping analysis, given the potential misuse of these substances in animal sports, there is an urgent demand for an allencompassing screening method to effectively identify these compounds. Objective: To develop a robust and sensitive high-resolution method for simultaneous screening of small peptides, corticosteroids, SARMs, and QADs using liquid chromatography accurate mass spectrometry in post-race urine samples. This method integrates a streamlined single-stage extraction approach, significantly enhancing efficiency and adaptability for screening drugs across various classes. Method: The method development and validation involved a comprehensive solid-phase extraction protocol, which included a sequential elution for corticosteroids, small peptides, SARMs, and QADs. Chromatographic separation was achieved using a reverse-phase C18 column, and the analysis was performed using liquid chromatography - high-resolution accurate mass spectrometry. Results: The developed method was validated using a selection of drugs representing each class. The method exhibited robustness and sensitivity, enabling the simultaneous screening of the specified drug classes. The flexibility inherent in the proposed extraction and analysis method allows for seamless integration of new drug candidates eliminating the need for method redevelopment. Conclusion: A versatile and effective screening method was successfully developed and validated for the simultaneous detection of small peptides, corticosteroids, SARMs, and QADs. The method's ability for retrospective analysis of emerging drugs using full scan HRMS enhances its utility. This method holds great promise across various fields where accurate and comprehensive drug screening is imperative.

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来源期刊

Current Analytical Chemistry 化学-分析化学

CiteScore

4.10

自引率

0.00%

发文量

审稿时长

9 months

期刊介绍： Current Analytical Chemistry publishes full-length/mini reviews and original research articles on the most recent advances in analytical chemistry. All aspects of the field are represented, including analytical methodology, techniques, and instrumentation in both fundamental and applied research topics of interest to the broad readership of the journal. Current Analytical Chemistry strives to serve as an authoritative source of information in analytical chemistry and in related applications such as biochemical analysis, pharmaceutical research, quantitative biological imaging, novel sensors, and nanotechnology.