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首页> 外文期刊>Journal of chromatography, B. Analytical technologies in the biomedical and life sciences >Structural elucidation of in vivo metabolites of penehyclidine in rats by the method of liquid chromatography-mass spectrometry, gas chromatography-mass spectrometry and isotope ion cluster
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Structural elucidation of in vivo metabolites of penehyclidine in rats by the method of liquid chromatography-mass spectrometry, gas chromatography-mass spectrometry and isotope ion cluster

机译:液相色谱-质谱联用,气相色谱-质谱联用和同位素离子簇方法对大鼠体内戊乙哌啶代谢产物进行结构解析

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摘要

The structural elucidation of metabolites of penehyclidine in rats, a novel anti-cholinergic drug, by the method of liquid chromatography-electrospray ionization mass spectrometry, gas chromatography-mass spectrometry with electron impact ion source and stable isotope ion cluster was described. Identification and elucidation of the phase I and phase II metabolites were performed by comparing the daughter ion pairs of stable isotope cluster, changes of the protonated molecular masses, full scan MSn spectra and retention times with those of the parent drug, penehyclidine and penehyclidine deuterium-labeled. Penehyclidine was easily biotransformed by the pathways of oxidative, hydroxylated, methoxylated and phase II conjugated reactions to form several metabolites that retained the some features of the parent molecules. Twelve metabolites (penehyclidine monoxide, trihydroxypenehyclidine, penehyclidine dioxide, hydroxypenehyclidine monoxide, dihydroxypenehyclidine, dihydroxypenehyclidine (position isomer), dihydroxypenehyclidine monoxide, trihydroxypenehyclidine, methoxypenehyclidine dioxide, dimethoxypenehyclidine, trihydroxymethoxypenehyclidine and glucuronide conjugated hydroxypenehyclidine) were identified. The results from electrospray ion and electron impact ion data with the stable isotope cluster showed the qualitative differences in the mass spectral patterns, suggesting that these technologies should be used in parallel to ensure Comprehensive metabolites detection and characterization. The described method has wide applicability to rapidly screen and provide structural information of metabolites. (C) 2008 Elsevier B.V. All rights reserved.
机译:通过液相色谱-电喷雾电离质谱,电子碰撞离子源和稳定同位素离子簇气相色谱-质谱联用的方法,对一种新的抗胆碱药大鼠戊乙奎啶的代谢产物进行了结构解析。通过比较稳定同位素簇的子离子对,质子化分子质量的变化,全扫描MSn谱和保留时间与母体药物戊乙奎啶和戊乙啶氘的比较,进行了I期和II期代谢物的鉴定和阐明。标记。通过氧化,羟基化,甲氧基化和II期共轭反应的途径,戊二烯易于生物转化,形成几种保留了母体分子某些特征的代谢产物。十二种代谢产物(一氧化苯丙啶,三羟基苯丙啶,二戊基吡啶二氧化物,一羟基苯丙啶一氧化物,二羟基苯丙啶,二羟基苯丙啶(位置异构体),二羟基苯丙啶一氧化氮,三羟基苯丙啶,甲氧基苯二甲酰二氧萘啶,二甲氧基苯丙啶,二甲氧基苯丙啶来自具有稳定同位素簇的电喷雾离子和电子碰撞离子数据的结果表明质谱图谱在质量上存在差异,这表明应并行使用这些技术以确保对代谢物进行全面检测和表征。所描述的方法具有广泛的适用性以快速筛选和提供代谢物的结构信息。 (C)2008 Elsevier B.V.保留所有权利。

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