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首页> 外文期刊>Saudi Pharmaceutical Journal >New bioanalytical microemulsion Electrokinetic chromatography method for the simultaneous determination of Trifluridine with its metabolites and Tipiracil in rat plasma: Application to pharmacokinetic studies
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New bioanalytical microemulsion Electrokinetic chromatography method for the simultaneous determination of Trifluridine with its metabolites and Tipiracil in rat plasma: Application to pharmacokinetic studies

机译:新型生物分析微乳液电动色谱法,用于同时测定Triflidine及大鼠等血浆中的代谢物和Tipiracil:药代动力学研究的应用

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A Microemulsion Electrokinetic Chromatography method coupled with diode array detector (MEEKC-DAD) was developed for the first time and found to be efficient, sensitive, and selective for the simultaneous analysis of Trifluridine (FTD), and its metabolites 5-(trifluoromethyl) uracil (FTY) and 5-carboxy-2′-deoxyuridine (5CDU), and Tipiracil (TIP) in rat plasma. Sample pre-treatment involved a simple protein precipitation from plasma using acetonitrile. The separation was achieved using a fused silica capillary (65?cm total length, 55?cm effective length and 50?μm i.d.) and a microemulsion solution consisted of 1.66% sodium dodecyl sulfate (SDS), 0.91% heptane, 6.61% 1-butanol, and 90.72% borate buffer (20?mM, pH 9.5). Electrophoretic separation was carried out at 20?°C and 20?kV. The samples were injected for 40?s at 20?mbar and detected simultaneously at 205?nm. The electrophoretic parameters indicated that the developed MEEKC-DAD method permitted complete resolution of the analytes within 13?min. The developed method was fully validated according to the FDA guidelines for bioanalytical method validation. The method was linear in the range 200–4000?ng/ml for FTD, FTY, 5CDU, and 100–1000?ng/ml for TIP. The intra/inter-day accuracy and precisions were ≤4% for all drugs. Extraction recovery and stability were also assessed and were within acceptable range. After being validated, the method was applied for the determination of the studied drugs in plasma samples collected from rats injected intraperitoneally with a combination of FTD and TIP. The results obtained were used to study the pharmacokinetics of FTD with its metabolite and TIP in rat plasma.
机译:一种微乳液电动色谱法与二极管阵列检测器(MEEKC-DAD)进行首次开发,发现是有效,敏感的,选择性,用于同时分析Trifluridine(FTD),及其代谢物5-(三氟甲基)尿嘧啶(FTY)和5-羧基-2'-脱氧尿苷(5CDU)和大鼠等离子体中的TIPIRACIL(尖端)。样品预处理涉及使用乙腈从等离子体中沉淀的简单蛋白质沉淀。使用熔融二氧化硅毛细管(65〜cm总长度,55℃有效长度和50μmid)和微乳液溶液和0.91%庚烷,0.91%庚烷,6.61%1-丁醇和90.72%的硼酸盐缓冲液(20?mm,pH9.5)。电泳分离在20℃和20 kV下进行。将样品在20μmbar以20×mbar注入40℃并在205℃下同时检测。电泳参数表明,发育的MEEKC-DAD方法允许在13℃内完成分析物的分析。根据生物分析方法验证的FDA指南完全验证开发的方法。该方法是线性的200-4000〜FTD,FTD,5CDU和100-1000〜100-1000〜100-1000Ω·Ng / ml的线性。所有药物的内部/日内准确度和精度≤4%。还评估提取恢复和稳定性,并且在可接受的范围内。经过验证后,施用该方法用于测定由FTD和尖端的组合腹膜内注入的大鼠收集的血浆样品中的研究中的药物。获得的结果用于研究FTD的药代动力学与大鼠等离子体中的代谢物和尖端。

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