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Comparative pharmacokinetics of icariin in plasma after oral administration of Er-Xian decoction or pure icariin in rats

机译:口服二仙汤或纯苦参素后大鼠血浆苦参素的比较药代动力学

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The present study was to investigate the pharmacokinetics of icariin in rat after oral administration of single dose of Er-xian decoction (EXD) and pure icariin. Blood samples were collected by orbital vein at time intervals after drug administration and the plasma concentrations of the studied components were determined by high performance liquid chromatography (HPLC) after the plasma protein was precipitated directly with acetonitrile. Icariin was successfully separated using a C18column with a UV detection at 270 nm and a mobile phase of acetonitrile–water with 0.1% H3PO4(35:65, v/v) pumped at 1.0 ml/min. The method had a lower limit of quantitation (LOQ) of 0.60 μg/ml for icariin with the limit of detection (LOD) 0.35 μg/ml, based on a signal-to-noise ratio of 3. The assay was linear over a range 0.667 to 42.67 μg/ml with coefficient of determination greater than 0.99 for analytes. The extraction recoveries was &80%. The method has shown tremendous reproducibility, with intra- and inter-day precision &4.9% (RSD), and has proved to be highly reliable for the analysis of plasma samples. The main pharmacokinetic parameters of icariin in rats after administration, EXD and icariin were processed by Das 2.0, while calculating the pharmacokinetic parameters of one compartment model. From the experimental results, the method had been applied successfully to pharmacokinetics of icariin in rat plasma after oral administration of pure icariin or EXD.
机译:本研究旨在研究口服单剂量的二仙汤(EXD)和纯净的蓖麻油素后大鼠体内番ari素的药代动力学。给药后的时间间隔通过眼眶静脉收集血样,血浆蛋白直接用乙腈沉淀后,用高效液相色谱法(HPLC)测定所研究成分的血浆浓度。使用C18色谱柱成功分离出伊卡瑞因,该色谱柱在270 nm处有UV检测,并以1.0 ml / min的速度泵入含有0.1%H3PO4(35:65,v / v)的乙腈-水流动相。基于信噪比3,该方法对大麻素的定量下限(LOQ)为0.60μg/ ml,检出限(LOD)为0.35μg/ ml。线性在0.667至42.67μg/ ml范围内,分析物的测定系数大于0.99。提取回收率> 80%。该方法显示出极大的可重复性,日内和日间精度<4.9%(RSD),并且被证明对于血浆样品的分析是高度可靠的。在给药后,用Das 2.0处理大鼠体内番泻素的主要药代动力学参数,EXD和番泻素,同时计算一个区室模型的药代动力学参数。从实验结果来看,该方法已成功地应用于口服纯icariin或EXD后icariin在大鼠血浆中的药代动力学。

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