积雪草酸大鼠体内药动学考察  被引量:6

Study on Pharmacokinetics of Asiatic Acid in Rats

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作  者:张雅雯[1] 尹丽娜[1] 梁泽华[2] 吴斌丽[1,2] 朱亮[1,2] 黄夏樱 王胜浩[1] 

机构地区:[1]浙江省医学科学院,杭州310013 [2]浙江中医药大学药学院,杭州310053

出  处:《中国现代应用药学》2015年第3期314-317,共4页Chinese Journal of Modern Applied Pharmacy

基  金:浙江省科技厅项目(2011F10048);浙江省新世纪151人才工程(第二层次);浙江省卫生高层次创新人才培养工程项目(2008);浙江省医学重点学科群建设资助项目(XKQ-010-001)

摘  要:目的 建立大鼠血浆中积雪草酸(asiatic acid,AA)的柱前衍生化HPLC,探讨AA在大鼠体内的药动学。方法 SD大鼠,♂,尾静脉注射AA(10 mg.kg 1),于给药后不同时间采取血浆,经DIKMA Proelut PLS柱固相萃取,柱前衍生化HPLC测定血浆中AA浓度(以甘草次酸为内标),药物统计软件(PKS 1.0)拟合统计药动学参数。结果 血药浓度在0.1~20μg.mL 1内线性良好(r=0.999 6),平均提取回收率为71.1~79.9%,日内、日间精密度RSD均〈13%,样品在20℃放置,经2次冻融循环后基本稳定。AA在大鼠体内药-时曲线符合一室开放模型,主要药动学参数为:tmax=2.0 min,Cmax=14.7μg.mL-1,t1/2=35.1 min,AUC0-t=217.0μg.min.mL 1,AUC0∞=234.3μg.min.mL 1。结论 AA在大鼠体内消除迅速,所建立的提取及柱前衍生化HPLC适用于体内AA的测定。OBJECTIVE To establish a sensitive precolumn derivatization HPLC method for determination of plasma concentration of asiatic acid(AA) and evaluate its pharmacokinetics characteristics in rats.METHODS The male SD rats were intravenously administrated AA by 10mg·kg-1.The plasma samples were taken at different times,concentrated by SPE method and determined by precolumn derivatization RP-HPLC method,the glycyrrhetinic acid was used as an internal standard.The pharmaeokinetie parameters were accessed by PKS 1.0.RESULTS Excellent liner relationship was obtained in the range of 0.1 to 20 μg·m L-1(r=0.999 6).The averang extraction recovery was 71.1%-79.9%.The intra- and inter-day RSDs were less than 13%.The samples were stabled at-20 ℃,and remained stable after twice freeze-thaw cycles.AA was fitted to a one compartment open model in rats,mainly pharmacokinetic parameters as follow: tmax=2.0min,Cmax=14.7 μg·m L-1,t1/2=35.1min,AUC0-t=217.0 μg·min·m L-1,AUC0-∞=234.3 μg·min·m L-1.CONCLUSION AA is disposed extensively and rapidly in rats.The method can be used to determine the concentration and to investigate the pharmacokinetics of AA in rats.

关 键 词:积雪草酸 血药浓度 固相萃取 一室模型 

分 类 号:R969.1[医药卫生—药理学]

 

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