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首页> 外文期刊>Biomedical Chromatography: An International Journal Devoted to Research in Chromatographic Methodologies and Their Applications in the Biosciences >Development of solid-phase microextraction coupled with liquid chromatography for analysis of tramadol in brain tissue using its molecularly imprinted polymer
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Development of solid-phase microextraction coupled with liquid chromatography for analysis of tramadol in brain tissue using its molecularly imprinted polymer

机译:用其分子印迹聚合物分析液相色谱法,用其分子印迹聚合物分析脑组织曲马多的液相色谱

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摘要

In this work, performance of a molecularly imprinted polymer (MIP) as a selective solid-phase microextraction sorbent for the extraction and enrichment of tramadol in aqueous solution and rabbit brain tissue, is described. Binding properties of MIPs were studied in comparison with their nonimprinted polymer (NIP). Ten milligrams of the optimized MIP was then evaluated as a sorbent, for preconcentration, in molecularly imprinted solid-phase microextraction (MISPME) of tramadol from aqueous solution and rabbit brain tissue. The analytical method was calibrated in the range of 0.004 ppm (4 ng mL(-1)) and 10 ppm (10 mu gmL(-1)) in aqueous media and in the ranges of 0.01 and 10 ppm in rabbit brain tissue, respectively. The results indicated significantly higher binding affinity of MIPs to tramadol, in comparison with NIP. The MISPME procedure was developed and optimized with a recovery of 81.12-107.54% in aqueous solution and 76.1691.20% in rabbit brain tissue. The inter-and intra-day variation values were < 8.24 and 5.06%, respectively. Finally the calibrated method was applied for determination of tramadol in real rabbit brain tissue samples after administration of a lethal dose. Our data demonstrated the potential of MISPME for rapid, sensitive and cost-effective sample analysis.
机译:在这项工作中,描述了分子印迹聚合物(MIP)作为选择性固相微萃取吸附剂,用于在水溶液和兔脑组织中提取和富集曲马多的选择性固相微萃取剂。研究了MIPS的结合特性与它们的非贴印聚合物(NIP)进行了研究。然后将10毫克优化的MIP作为吸附剂评估为预浓缩,以来自水溶液和兔脑组织的曲马多的分子印迹固相微萃取(MISPME)。分析方法分别在0.004ppm(4ng ml(-1))和10ppm(10μgmml(-1))中校准的分析方法分别在兔脑组织中的0.01和10ppm的范围内。结果表明,与辊隙相比,MIPS对曲马多的结合具有显着更高的亲和力。 MISPME程序开发并优化,在水溶液中的回收率为81.12-107.54%,兔脑组织中的76.1691.20%。间间变异值分别为<8.24和5.06%。最后,应用校准方法在施用致死剂量后施用真实兔脑组织样品中的曲马多。我们的数据展示了MISPME的潜力,用于快速,敏感和经济高效的样本分析。

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