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为兴奋剂检测目的鉴定快速骨骼肌肌钙蛋白激活剂替拉米特和瑞地米特的人体代谢物。

Identification of human metabolites of fast skeletal troponin activators Tirasemtiv and Reldesemtiv for doping control purposes.

作者信息

Euler Luisa, Deinert Kim, Wagener Felicitas, Walpurgis Katja, Thevis Mario

机构信息

Center for Preventive Doping Research Institute of Biochemistry, German Sport University Cologne, Cologne, Germany.

Technical University of Kaiserslautern, Kaiserslautern, Germany.

出版信息

Drug Test Anal. 2025 Jun;17(6):812-824. doi: 10.1002/dta.3786. Epub 2024 Aug 13.

Abstract

The fast skeletal troponin activators (FSTAs) Reldesemtiv and Tirasemtiv were developed for patients suffering from neuro-degenerative diseases of the motor nervous system, e.g. amyotrophic lateral sclerosis (ALS). The drug candidates can increase the sensitivity of troponin C to calcium by selectively activating the troponin complex resulting in increased skeletal muscle contraction. Although the development of the drug candidates is currently discontinued because of missed end points in phase III clinical studies with patients with ALS, phase I clinical trials showed an increase in muscle contraction force in healthy humans. This effect could be abused by athletes to enhance performance in sports. As the substances are listed on the 2024 edition of the World Anti-Doping Agency's Prohibited List, the aim of this study was to identify and characterize metabolites of Reldesemtiv and Tirasemtiv to ensure their reliable identification in doping control analyses. The biotransformation of the drug candidates was studied in vitro using pooled human liver microsomes and 3D cultivated human hepatic cells of the cell line HepaRG, yielding a total of 11 metabolites of Reldesemtiv and eight of Tirasemtiv. In addition, a human elimination study was conducted to investigate the metabolism and elimination profile of Tirasemtiv and Reldesemtiv in vivo, suggesting the N-glucuronide of Tirasemtiv and hydroxylated 3-fluoro-2-(3-fluoro-1-methylcyclobutyl)pyridine as well as its glucuronide as suitable target analytes for routine doping controls. Applying a validating HPLC-MS/MS method, optimized to detect Reldesemtiv and Tirasemtiv in human urine, microdosing (50 μg) of each substance was traceable for 24-72 h.

摘要

快速骨骼肌肌钙蛋白激活剂(FSTAs)瑞地西美和替拉西美是为患有运动神经系统神经退行性疾病(如肌萎缩侧索硬化症,ALS)的患者开发的。这些候选药物可以通过选择性激活肌钙蛋白复合物来增加肌钙蛋白C对钙的敏感性,从而导致骨骼肌收缩增强。尽管由于ALS患者的III期临床研究未达到终点,目前已停止这些候选药物的开发,但I期临床试验显示健康人肌肉收缩力有所增加。运动员可能会滥用这种效果来提高运动成绩。由于这些物质被列入世界反兴奋剂机构2024年版的《禁用清单》,本研究的目的是鉴定和表征瑞地西美和替拉西美的代谢物,以确保在兴奋剂检测分析中能够可靠地识别它们。使用人肝微粒体池和HepaRG细胞系的3D培养人肝细胞在体外研究了候选药物的生物转化,共产生了11种瑞地西美的代谢物和8种替拉西美的代谢物。此外,还进行了一项人体消除研究,以调查替拉西美和瑞地西美在体内的代谢和消除情况,表明替拉西美的N-葡萄糖醛酸苷、羟基化的3-氟-2-(3-氟-1-甲基环丁基)吡啶及其葡萄糖醛酸苷是常规兴奋剂检测的合适目标分析物。应用一种经过验证的HPLC-MS/MS方法,该方法经过优化可检测人尿中的瑞地西美和替拉西美,每种物质微剂量给药(50μg)后可在24 - 72小时内被检测到。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/117b/12151715/1fc770066b9b/DTA-17-812-g001.jpg

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