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首页> 外文期刊>Therapeutic Drug Monitoring >Issues in methodology and applications for therapeutic drug monitoring of fluoxetine and norfluoxetine enantiomers.
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Issues in methodology and applications for therapeutic drug monitoring of fluoxetine and norfluoxetine enantiomers.

机译:氟西汀和诺氟西汀对映异构体的治疗药物监测方法和应用中的问题。

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摘要

A standardization of the analytical procedures for monitoring of fluoxetine and norfluoxetine enantiomers is described. Simultaneous determination of fluoxetine and norfluoxetine enantiomers in plasma and serum was performed by high-performance liquid chromatography with a chiral stationary phase, using ultraviolet absorbance detection. The analytes were extracted from the biologic matrix by alkalinization with NaOH and solid-phase extraction. Stability studies were conducted in EDTA, lithium-heparinized plasma and in serum spiked with the analytes stored at +4 degrees C for 1 week and at -20 degrees C for 1 month. Furthermore, stability studies in NaOH and in the extraction solvents were executed. Using this methodology, EDTA plasma is the most suitable matrix for drug monitoring, even if the storage should not exceed 3 weeks at -20 degrees C. Furthermore, the biologic sample should be left in NaOH for a short time before solid-phase extraction to prevent a degradation of matrix, which would interfere with the chromatographic analysis.
机译:描述了用于监测氟西汀和去氟西汀对映体的分析程序的标准化。高效液相色谱-手性固定相-紫外吸收检测法同时测定血浆和血清中氟西汀和诺氟西汀对映体的含量。通过用NaOH碱化和固相萃取从生物基质中提取分析物。在EDTA,锂肝素化血浆和掺有分析物的血清中进行了稳定性研究,分析物分别在+4摄氏度和1摄氏度,在-20摄氏度的条件下储存。此外,还进行了在NaOH和萃取溶剂中的稳定性研究。使用这种方法,即使在-20摄氏度下储存不应超过3周,EDTA血浆也是最适合进行药物监测的基质。此外,在将固相萃取物提取到NaOH中之前,应将生物样品在NaOH中放置一小段时间。防止基质降解,而基质降解会干扰色谱分析。

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