首页> 外文期刊>Biomedical Chromatography: An International Journal Devoted to Research in Chromatographic Methodologies and Their Applications in the Biosciences >Simultaneous determination of fluoxetine and its major active metabolite norfluoxetine in human plasma by LC-MS/MS using supported liquid extraction
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Simultaneous determination of fluoxetine and its major active metabolite norfluoxetine in human plasma by LC-MS/MS using supported liquid extraction

机译:使用负载液提取的LC-MS / MS同时测定人血浆中的氟苯氧脲及其主要活性代谢物NORFOXETIN

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摘要

A rapid, sensitive and selective bioanalytical method was developed for the simultaneous determination of fluoxetine and its primary metabolite norfluoxetine in human plasma. Sample preparation was based on supported liquid extraction (SLE) using methyl tert-butyl ether to extract the analytes from human plasma. Chromatography was performed on a Synergi 4μ polar-RP column using a fast gradient. The ionization was optimized using ESI (+) and selectivity was achieved by tandem mass spectrometric analysis using MRM functions, m/z 310→44 for fluoxetine, m/z 296→134 for norfluoxetine and m/z 315→44 for fluoxetine-d 5 (internal standard). The method is linear over the range of 0.05-20ng/mL (using a human plasma sample volume of 0.1mL) with a coefficient determination of greater than 0.999. The method is accurate and precise with intra-batch and inter-batch accuracy (%bias) of ±15% and precision (%CV) of 15% for both analytes. A run time of 4min means a high throughput of samples can be achieved. To our knowledge, this method appears to be the most sensitive one reported so far for the quantitation of fluoxetine and norfluoxetine and can be used for routine therapeutic drug monitoring or pharmacokinetic studies.
机译:开发了一种快速,敏感和选择性生物分析方法,用于同时测定人血浆中氟西汀及其原发性代谢物。样品制备基于使用甲基叔丁基醚的负载型液体萃取(SLE),以从人血浆中提取分析物。使用快速梯度在Synergi4μg100峰值柱上进行色谱。使用ESI(+)优化电离,通过使用MRM函数,M / Z 310→44用于氟西汀的M / Z 310→44,用于NORFLUOXETINE和M / Z 315→44用于氟西汀-D的M / Z 310→134,实现选择性。 5(内标)。该方法在0.05-20ng / ml的范围内(使用人血浆样品体积为0.1ml),系数测定大于0.999。该方法具有精确且精确地具有批次内的间歇性和间歇性精度(%偏压),<±15%和β15%的精度(%CV)。 4分钟的运行时间意味着可以实现高吞吐量。为了我们的知识,这种方法似乎是迄今为止最敏感的,以氟西汀和氟诺昔汀的定量报告,可用于常规治疗药物监测或药代动力学研究。

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