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采用荧光偏振免疫分析(FPIA)和酶免疫分析(EIA)进行尿液中α-羟基三唑仑筛查,并通过气相色谱/质谱联用(GC/MS)进行确证。

Urinary screening for alpha-OH triazolam by FPIA and EIA with confirmation by GC/MS.

作者信息

Fraser A D, Bryan W, Isner A F

机构信息

Toxicology Laboratory, Victoria General Hospital, Halifax, Nova Scotia, Canada.

出版信息

J Anal Toxicol. 1992 Nov-Dec;16(6):347-50. doi: 10.1093/jat/16.6.347.

Abstract

Triazolam is a very short-acting triazolobenzodiazepine with sedative-hypnotic properties. Approximately 2% of an oral dose is excreted unchanged in the urine. The major urinary metabolite is alpha-hydroxytriazolam glucuronide (70% of the dose). The objective of this study was to characterize the reactivity of alpha-hydroxytriazolam in the urine benzodiazepine assay by fluorescence polarization immunoassay (FPIA; Abbott TDx) in comparison with enzyme immunoassay (EIA; Syva EMIT d.a.u. benzodiazepine assay). alpha-OH triazolam at 300 ng/mL gave a response equivalent to the 200-ng/mL nordiazepam Abbott calibrator. In the EMIT assay, alpha-OH triazolam gave a response equivalent to the 300-ng/mL calibrator (Syva) at 100-200 ng/mL. Both immunoassays gave positive results in 9 out of 9 urine specimens collected from individuals receiving triazolam. Confirmation was performed by analyzing for alpha-OH triazolam after enzymatic hydrolysis and formation of a TMS derivative for GC/MS. All urine specimens were positive for alpha-OH triazolam. In conclusion, both the FPIA and EIA immunoassay screening assays are acceptable for detecting the presence of alpha-OH triazolam in the urine of patients receiving therapeutic doses of triazolam.

摘要

三唑仑是一种具有镇静催眠特性的超短效三唑并苯二氮䓬类药物。口服剂量中约2%以原形经尿液排出。主要的尿液代谢产物是α-羟基三唑仑葡萄糖醛酸苷(占剂量的70%)。本研究的目的是通过荧光偏振免疫分析法(FPIA;雅培TDx)与酶免疫分析法(EIA;西瓦EMIT d.a.u.苯二氮䓬类药物分析法)比较,来表征尿液苯二氮䓬类药物分析中α-羟基三唑仑的反应性。300 ng/mL的α-OH三唑仑产生的反应相当于200 ng/mL的去甲西泮雅培校准品。在EMIT分析中,100 - 200 ng/mL的α-OH三唑仑产生的反应相当于300 ng/mL的校准品(西瓦)。两种免疫分析法对从接受三唑仑治疗的个体收集的9份尿液标本中的9份均给出了阳性结果。通过酶促水解后分析α-OH三唑仑并形成用于气相色谱/质谱联用(GC/MS)的TMS衍生物进行确证。所有尿液标本中α-OH三唑仑均呈阳性。总之,FPIA和EIA免疫分析筛查法均可用于检测接受治疗剂量三唑仑的患者尿液中α-OH三唑仑的存在。

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