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首页> 外文期刊>Journal of Chromatography, Biomedical Applications >Simultaneous determination of fluoxetine and its metabolite p-trifluoromethylphenol in human liver microsomes using a gas chromatographic-electron-capture detection procedure
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Simultaneous determination of fluoxetine and its metabolite p-trifluoromethylphenol in human liver microsomes using a gas chromatographic-electron-capture detection procedure

机译:气相色谱-电子捕获检测法同时测定人肝微粒体中的氟西汀及其代谢物对三氟甲基苯酚

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An gas chromatography-electron-capture detection method has been developed for simultaneous determination of fluoxetine and p-trifluoromethylphenol (TFMP), and O-dealkylated metabolite of fluoxetine in human liver microsomes. Prior to the analysis, aliquots of alkalinized microsomal mixture were extracted with ethyl acetate solvent containing acetonitrile (10%, v/v) and the derivatizing reagent, pentafluorobenzenesulfonyl chloride (0.1%, v/v). The organ phase was retained and taken to dryness, the residue was reconstituted in methanol, and the aliquot of extracts was injected directly into a gas chromatograph equipped with an electron-capture detector. 2,4-Dichlorophenol was added to the initial incubation mixture and carried through the procedure as the internal standard. The method provided the mean recoveries of up to 103% for fluoxetine and 104% for TEMP. Acceptable relative standard deviations were found for both within-run and day-to-day assays. The practical limit of detection (signal-to-noise ratio = 3) was 1.62 ng/ml for TFMP and 6.92 ng/ml for fluoxetine in human liver microsomes, and the limit of quantitation was 8.1 pg for TFMP and 34.6 pg for fluoxetine. The assay is rapid and sensitive and has been applied successfully to simultaneous quantification of fluoxetine and TFMP in human liver microsomes with different CYP2C19 genotypes.
机译:已经开发了一种气相色谱-电子捕获检测方法,用于同时测定人肝微粒体中的氟西汀和对三氟甲基苯酚(TFMP)和氟西汀的O-脱烷基代谢产物。在分析之前,用含乙腈(10%,v / v)和衍生试剂五氟苯磺酰氯(0.1%,v / v)的乙酸乙酯溶剂萃取碱化的微粒体混合物的等分试样。保留器官相并干燥,将残余物在甲醇中重构,并将提取的等分试样直接注入配备有电子捕获检测器的气相色谱仪中。将2,4-二氯苯酚添加到初始孵育混合物中,并按照该程序作为内标。该方法对氟西汀的平均回收率高达103%,对TEMP的回收率高达104%。对于运行内和日常测定均发现可接受的相对标准偏差。人肝微粒体的实际检测极限(信噪比= 3)为TFMP为1.62 ng / ml,氟西汀为6.92 ng / ml,TFMP的定量极限为8.1 pg,氟西汀的定量极限为34.6 pg。该方法快速,灵敏,已成功用于同时定量具有不同CYP2C19基因型的人肝微粒体中的氟西汀和TFMP。

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