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首页> 外文期刊>Drug testing and analysis >Mass spectrometric characterization of the hypoxia-inducible factor (HIF) stabilizer drug candidate BAY 85-3934 (molidustat) and its glucuronidated metabolite BAY-348, and their implementation into routine doping controls
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Mass spectrometric characterization of the hypoxia-inducible factor (HIF) stabilizer drug candidate BAY 85-3934 (molidustat) and its glucuronidated metabolite BAY-348, and their implementation into routine doping controls

机译:缺氧诱导因子(HIF)稳定剂药物候选湾85-3934(Molidustat)及其葡萄糖化代谢物湾-348的质谱表征及其在常规掺杂控制中的实施

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摘要

The development of new therapeutics potentially exhibiting performance-enhancing properties implicates the risk of their misuse by athletes in amateur and elite sports. Such drugs necessitate preventive anti-doping research for consideration in sports drug testing programmes. Hypoxia-inducible factor (HIF) stabilizers represent an emerging class of therapeutics that allows for increasing erythropoiesis in patients. BAY 85-3934 is a novel HIF stabilizer, which is currently undergoing phase-2 clinical trials. Consequently, the comprehensive characterization of BAY 85-3934 and human urinary metabolites as well as the implementation of these analytes into routine doping controls is of great importance. The mass spectrometric behaviour of the HIF stabilizer drug candidate BAY 85-3934 and a glucuronidated metabolite (BAY-348) were characterized by electrospray ionization-(tandem) mass spectrometry (ESI-MS(/MS)) and multiple-stage mass spectrometry (MSn). Subsequently, two different laboratories established different analytical approaches (one each) enabling urine sample analyses by employing either direct urine injection or solid-phase extraction. The methods were cross-validated for the metabolite BAY-348 that is expected to represent an appropriate target analyte for human urine analysis. Two test methods allowing for the detection of BAY-348 in human urine were applied and cross-validated concerning the validation parameters specificity, linearity, lower limit of detection (LLOD; 1-5ng/mL), ion suppression/enhancement (up to 78%), intra- and inter-day precision (3-21%), recovery (29-48%), and carryover. By means of ten spiked test urine samples sent blinded to one of the participating laboratories, the fitness-for-purpose of both assays was provided as all specimens were correctly identified applying both testing methods. As no post-administration study samples were available, analyses of authentic urine specimens remain desirable. Copyright (c) 2016 John Wiley & Sons, Ltd.
机译:新的治疗方法的发展可能表现出绩效增强的属性介绍了运动员在业余和精英体育运动中滥用滥用的风险。这种药物需要预防性的反兴奋剂研究,以考虑体育药物检测计划。缺氧诱导因子(HIF)稳定剂代表新出现的治疗剂,允许增加患者的红细胞病毒。 Bay 85-3934是一种新型HIF稳定剂,目前正在进行2阶段临床试验。因此,海湾85-3934和人类尿代谢物的综合表征以及将这些分析物的实施进入常规掺杂对照的情况非常重要。通过电喷雾电离(串联)质谱(ESI-MS(/ MS))和多阶段质谱( MSN)。随后,两种不同的实验室建立了通过使用直接尿液注射或固相萃取来实现不同的分析方法(每一个),从而实现尿液样品分析。对于代谢物湾-348的方法是交叉验证的,所述代谢物湾-348预期代表适当的人类尿液分析的目标分析物。允许检测人类尿液中Bay-348的两种测试方法,并交叉验证有关验证参数特异性,线性度,检测下限(LLOD; 1-5ng / ml),离子抑制/增强(高达78 %),内部和日间精度(3-21%),恢复(29-48%)和携带。借助于十个尖刺的测试尿液样本被蒙蔽到参与实验室之一,提供了两种测定的适应性,因为所有标本都被正确鉴定了应用两种测试方法。由于没有可用后给药后的研究样品,所以尿样的分析仍然是理想的。版权所有(c)2016 John Wiley&Sons,Ltd。

著录项

  • 来源
    《Drug testing and analysis 》 |2017年第2期| 共7页
  • 作者单位

    German Sport Univ Cologne Ctr Prevent Doping Res Inst Biochem Sportpk Muengersdorf 6 D-50933;

    Agence Francaise Lutte Dopage AFLD 143 Ave Roger Salengro F-92290 Chatenay Malabry France;

    Agence Francaise Lutte Dopage AFLD 143 Ave Roger Salengro F-92290 Chatenay Malabry France;

    Agence Francaise Lutte Dopage AFLD 143 Ave Roger Salengro F-92290 Chatenay Malabry France;

    German Sport Univ Cologne Ctr Prevent Doping Res Inst Biochem Sportpk Muengersdorf 6 D-50933;

    Bayer Pharma AG Aprather Weg D-42096 Wuppertal Germany;

    German Sport Univ Cologne Ctr Prevent Doping Res Inst Biochem Sportpk Muengersdorf 6 D-50933;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 药学 ;
  • 关键词

    sport; doping; mass spectrometry; HIF stabilizer;

    机译:运动;掺杂;质谱;HIF稳定剂;

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