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Determination of antifilarial compound UMF-078 and its metabolites in plasma by high-performance liquid chromatography
Affiliation:1. Department of Natural Sciences, Fibre Science and Communication Network (FSCN), Mid Sweden University, SE-851 70 Sundsvall, Sweden;2. Metso Panelboard AB, Department of Research, Technology and Development (RTD), SE-851 50 Sundsvall, Sweden;1. Department of Chemical Engineering, National Taiwan University, Roosevelt Road, Taipei 10617, Taiwan;2. Department of Physics and Materials Science and Engineering, Jaypee Institute of Information Technology University, Noida 201307, India;3. Photovoltaics Technology Center, Industrial Technology Research Institute, Hsin-Chu, Taiwan;1. Université de Toulouse, INPT, UPS, Laboratoire de Génie Chimique, 4, Allée Emile Monso, F-31030 Toulouse, France;2. CNRS, Laboratoire de Génie Chimique, F-31030 Toulouse, France
Abstract:UMF-078, methyl (±)-5-(α-amino-4-fluorobenzyl)benzimidazol-2-yl]carbamate, is a new antifilarial compound being developed by the World Health Organization. In the present study, a HPLC method for the simultaneous estimation of UMF-078 and its metabolites (flubendazole, decarbamoylated flubendazole, UMF060 and decarbamoylated UMF-060) in plasma was developed, validated and applied to pharmacokinetic studies. Linearity was observed between 20 and 1000 ng/ml for decarbamoylated UMF-060 and between 10 and 500 ng/ml for other analytes. Recoveries were consistent over the concentration ranges studied for all the analytes. Variations in intra- and inter-batch accuracy and precision were within acceptable limits of ±20% at the lowest limit of quantitation, whereas at higher concentrations it was ±15%. The analytes showed stability up to two freeze–thaw cycles in plasma. No degradation was observed for any of the analytes even after 72 h of storing the dry plasma extracts at −30°C. The assay method was employed to study the pharmacokinetics of hydrochloride salt of UMF-078 in rats. The parent compound and its metabolites viz: decarbamoylated UMF-060, UMF-060 and flubendazole were quantitated in serum and the compounds could be monitored up to 168 h post-dose.
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