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On‐line sample stacking and short‐end injection CE for the determination of fluoxetine and norfluoxetine in plasma: Method development and validation using experimental designs
Author(s) -
Lu ChiaChia,
Jong YuhJyh,
Ferrance Jerome,
Ko WeiKung,
Wu ShouMei
Publication year - 2007
Publication title -
electrophoresis
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.666
H-Index - 158
eISSN - 1522-2683
pISSN - 0173-0835
DOI - 10.1002/elps.200700187
Subject(s) - chromatography , chemistry , analytical chemistry (journal) , central composite design , stacking , resolution (logic) , methanol , pharmacokinetics , metabolite , response surface methodology , pharmacology , biochemistry , organic chemistry , artificial intelligence , computer science , medicine
A short‐end injection CE method combining field‐amplified sample stacking (FASS) is presented for the analysis of fluoxetine (FL) and norfluoxetine in plasma. In this study, FASS enhanced the sensitivity about 1100‐fold, while short‐end injection reduced the analysis time to less than 4 min. Parameters involved in the separations were investigated using a central composite design (CCD) and response surface methodology to optimize the separation conditions in a total of only 32 runs. Samples injected into the capillary for 99.9 s at a voltage of –5 kV were stacked in a water plug (0.5 psi, 9 s). Baseline resolution of FL and its major metabolite was achieved using a BGE formulation consisting of phosphate–triethanolamine at low pH, and a separation voltage of –10 kV. Five percent methanol was added as organic modifier to enhance selectivity and resolution. The linear range was between 10 and 500 ng/mL ( r >0.9946), covering the expected plasma therapeutic ranges. The LOD in plasma were 4 ng/mL (S/N = 3), a value comparable to that obtained using LC‐MS, showing the success of the on‐line stacking technique. Our method was also successfully validated in quantification and pharmacokinetic studies with three volunteer plasma samples and could be applied to pharmacogenetic studies.

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