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首页> 外文期刊>Forensic science international >Stereoselective analyses of selegiline metabolites: possible urinary markers for selegiline therapy.
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Stereoselective analyses of selegiline metabolites: possible urinary markers for selegiline therapy.

机译:司来吉兰代谢产物的立体选择性分析:司来吉兰治疗的可能尿液标志物。

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摘要

The stereoselective analysis of selegiline metabolites in human urine and plasma by gas chromatography using the chiral column with the non-chiral reagent was investigated for the differentiation of selegiline therapy from the methamphetamine (MA) abuse. This method gave clear separations of MA and amphetamine (AM) isomers without any artifactual optical-opposite peaks due to the reagent. After the administration of selegiline tablets, desmethylselegiline (DMS), MA and AM were observed as (-)-isomers in the urine and plasma. Within the first 48 h after dosing, approximately 40% of selegiline administered was excreted in urine as these three metabolites. The parent drug, selegiline, was not detected in any urine or plasma samples. On the other hand, MA and AM were observed only as (+)-isomers in the urine of MA abusers. For the distinction of selegiline users from street MA abusers in urinalysis, (-)-DMS, a specific metabolite of selegiline, was not a suitable marker. (-)-DMS rapidly disappeared from urine and was excreted only 1% of the given dose. By the moment analysis with the trapezoidal integration, the mean residence times of (-)-DMS in plasma and urine were 2.7 and 3.8 h, respectively, which were 5-20 times shorter than those of (-)-MA or (-)-AM. The values of AM/MA in the urine increased from 0.24 to 0.67 (r = 0.857) along with time after the selegiline administration. This ratio was not a sufficient marker to differentiate selegiline users from MA abusers, although the values of AM/MA in 74% of MA abusers were less than 0.24. The present GC technique improved the chiral analyses of MA and AM. This chiral analysis is the most useful technique to avoid the misinterpretation in the discrimination between clinical selegiline therapy and illicit MA use.
机译:使用手性色谱柱和非手性试剂,通过气相色谱法对人尿和血浆中的司来吉兰代谢产物进行了立体选择性分析,研究了司来吉兰疗法与甲基苯丙胺滥用之间的区别。此方法可清晰分离出MA和苯丙胺(AM)异构体,而没有由于试剂造成的任何人为的光学相反峰。给予司来吉兰片剂后,在尿液和血浆中观察到去甲基司来吉兰(DMS),MA和AM为(-)异构体。在给药后的第一个48小时内,大约有40%的司来吉兰作为这三种代谢物从尿中排出。在任何尿液或血浆样品中均未检测到母体药物司来吉兰。另一方面,在MA滥用者的尿液中仅观察到MA和AM为(+)-异构体。为了在尿液分析中将司来吉兰使用者与街头MA滥用者区分开来,司来吉兰的特定代谢产物(-)-DMS不是合适的标记物。 (-)-DMS迅速从尿液中消失,仅排泄给定剂量的1%。通过梯形积分的矩分析,(-)-DMS在血浆和尿液中的平均停留时间分别为2.7和3.8 h,比(-)-MA或(-)短5-20倍-上午。服用司来吉兰后,尿液中的AM / MA值从0.24升高到0.67(r = 0.857)。尽管有74%的MA滥用者的AM / MA值小于0.24,但该比率不足以区分司来吉兰使用者和MA滥用者。目前的气相色谱技术改进了MA和AM的手性分析。这种手性分析是避免临床司来吉兰疗法与非法使用MA之间的误解的最有用技术。

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