Bioanalysis of drugs by liquid-phase microextraction coupled to separation techniques |
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Authors: | Pedersen-Bjergaard Stig Rasmussen Knut Einar |
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Institution: | School of Pharmacy, University of Oslo, P.O. Box 1068, Blindern, 0316 Oslo, Norway. stig.pedersen-bjergaard@farmasi.uio.no |
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Abstract: | The demand for automation of liquid-liquid extraction (LLE) in drug analysis combined with the demand for reduced sample preparation time has led to the recent development of liquid-phase microextraction (LPME) based on disposable hollow fibres. In LPME, target drugs are extracted from aqueous biological samples, through a thin layer of organic solvent immobilised within the pores of the wall of a porous hollow fibre, and into an microl volume of acceptor solution inside the lumen of the hollow fibre. After extraction, the acceptor solution is subjected directly to a final analysis either by high performance liquid chromatography (HPLC), capillary electrophoresis (CE), mass spectrometry (MS), or capillary gas chromatography (GC) without any further treatments. Hollow fibre-based LPME may provide high enrichment of drugs and excellent sample clean-up, and probably has a broad application potential within the area of drug analysis. This review focuses on the principle of LPME, and recent applications of three-phase, two-phase, and carrier mediated LPME of drugs from plasma, whole blood, urine, and breast milk. |
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Keywords: | Liquid-phase microextraction Hollow fibres Drug analysis Plasma Whole blood Urine Breast milk |
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