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Enantioselective disposition of (R)-salmeterol and (S)-salmeterol in urine following inhaled dosing and application to doping control

机译:在吸入剂量后尿液中(R)-Salmeterol和(S)-Salmeterol的映射性配置和掺杂对照

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摘要

Salmeterol (USAN, INN, BAN) is a long-acting beta2-adrenoceptor agonist (LABA) widely used in the treatment of airways disease. Although salmeterol is permitted via inhalation by athletes and supratherapeutic dosing may enhance performance, no urine threshold has been established by the World Anti-Doping Agency (WADA). Salmeterol is a chiral compound consisting of (R)and (S)-enantiomers, normally administered as racemic (rac-) mixture via inhalation. Levels of rac-salmeterol in urine are often below detectable levels and there is surprisingly little information regarding the enantioselectivity of salmeterol pharmacokinetics. In this study, subjects inhaled either 50 (n = 6) or 200 mu g (n = 4; generally regarded as maximum therapeutic dose) of salmeterol and urine was then collected for 24 h and analyzed by enantioselective ultra performance liquid chromatography-tandem mass spectrometry (UPLC-MS/MS). Maximum rac-salmeterol urine concentrations were obtained at 2 h for both doses with medians of 0.084 ng/mL after the 50 mu g dose and 2.1 ng/mL after the 200 mu g dose, with an individual maximum of 5.7 ng/mL. Levels were detectable at 24h for both doses. Salmeterol displayed enantioselective pharmacokinetics, with amean +/- SD log (S):(R) = 0.055 +/- 0.025 (P < 0.0001) equivalent to (S):(R) of 1.13. In conclusion, rac-salmeterol by inhalation exhibits modest enantioselectivity in urine following single dose administration and can be detected following a single 50 mu g dose for up to 24 h after inhalation. The present findings are of relevance if a urine threshold limit is to be introduced for salmeterol on the list of prohibited substances. The application of an enantiomer ratio analysis may offer improved discriminatory detection capability for doping control analysis applications. Copyright (C) 2016 John Wiley & Sons, Ltd.
机译:Salmeterol(Usan,Inn,Ban)是一种长效的β2-adrenceptor激动剂(Laba),广泛用于治疗气道疾病。虽然运动员的吸入允许Salmeterol和Supratherapeutic Supys可能会增强性能,但世界反兴奋剂(WADA)没有建立尿液阈值。 Salmeterol是一种由(R)和(S) - 托体组成的手性化合物,通常通过吸入作为外消旋(RAC-)混合物给药。尿液中Rac-Salmeterol的水平往往低于可检测的水平,并且令人惊讶地存在关于Salmeterol药代动力学的对映射性的信息。在该研究中,然后收集研磨50(n = 6)或200μg(n = 4;通常被认为是最大治疗剂量)的Salmeterol和尿液的受试者进行24小时,并通过对映选择性的超级性能液相色谱 - 串联质量分析光谱法(UPLC-MS / MS)。在200μg剂量和200μg剂量后的50μg剂量和2.1ng / ml之后,在2小时内获得最大RAC-SALMETEROL尿液浓度。两种剂量的24小时可检测到水平。 Salmeterol展示了映选择性药代动力学,AMEAN +/-SD log(s):( r)= 0.055 +/- 0.025(p <0.0001)相当于(s):( r)为1.13。总之,通过吸入的Rac-Salmeterol在单剂量给药后吸入在尿液中表现出适度的对映选择性,并且在吸入后,可以在单个50μg剂量后检测到高达24小时后检测。如果要在禁止物质清单上为Salmeterol引入唾液阈值限制,则目前的结果具有相关性。对映重分析的施用可以为掺杂控制分析应用提供改进的歧视性检测能力。版权所有(c)2016 John Wiley&Sons,Ltd。

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