Pharmacokinetics and Bioavailability Study of 23-Acetyl Alisol B in Rats

LUO Yong-dong; LI Xiao-yan; QIU Li-li; XU Wen; WU Shui-sheng

doi:10.13422/j.cnki.syfjx.2010.12.050

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Pharmacokinetics and Bioavailability Study of 23-Acetyl Alisol B in Rats

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- Pharmacokinetics and Bioavailability Study of 23-Acetyl Alisol B in Rats
- Chinese Journal of Experimental Traditional Medical Formulae Vol. 16, Issue 12, Pages: 172-175(2010)
- 作者机构：
  
  福建中医药大学药学院方剂重点学科
- 作者简介：
- 基金信息：
- DOI：10.13422/j.cnki.syfjx.2010.12.050
  CLC： R285
- Published：2010
- 稿件说明：
移动端阅览
[1]罗永东,李小艳,邱丽莉,许文,吴水生.23-乙酰泽泻醇B大鼠体内药动学和生物利用度研究[J].中国实验方剂学杂志,2010,16(12):172-175.

LUO Yong-dong, LI Xiao-yan, QIU Li-li, et al. Pharmacokinetics and Bioavailability Study of 23-Acetyl Alisol B in Rats[J]. Chinese journal of experimental traditional medical formulae, 2010, 16(12): 172-175.
[1]罗永东,李小艳,邱丽莉,许文,吴水生.23-乙酰泽泻醇B大鼠体内药动学和生物利用度研究[J].中国实验方剂学杂志,2010,16(12):172-175. DOI： 10.13422/j.cnki.syfjx.2010.12.050.

LUO Yong-dong, LI Xiao-yan, QIU Li-li, et al. Pharmacokinetics and Bioavailability Study of 23-Acetyl Alisol B in Rats[J]. Chinese journal of experimental traditional medical formulae, 2010, 16(12): 172-175. DOI： 10.13422/j.cnki.syfjx.2010.12.050.

摘要

目的:对泽泻中主要成分23-乙酰泽泻醇B进行不同给药方式的药代动力学和口服生物利用度研究。方法:大鼠分别注射和灌服23-乙酰泽泻醇B

于不同时间点采血;采用HPLC-UV法检测血浆中23-乙酰泽泻醇B

流动相为乙腈-水（80∶20）

检测波长210 nm

流速1.0 mL·min-1;绘制药时曲线

建立药代动力学模型

计算药动学参数和绝对生物利用度（F）。结果:主要药动学参数为口服:Tmax（122.15±15.23）min

Cmax（9.89±0.87）mg·L-1

t1/2（58.72±6.23）min

AUC0-t（1 854.970±142.31）μg.min·mL-1

AUC0-∞（1 875.81±144.27）μg.min·mL-1

CL/F（2.89±0.13）mL·min-1;静脉注射:Tmax（10.04±0.78）min

Cmax（42.59±3.47）μg·mL-1

t1/2（32.05±2.53）min

AUC0-t（2 810.08±178.70）μg.min-1·mL-1

AUC0-∞（2 812.41±224.63）μg·min-1·mL-1

CL/F（1.74±0.54）mL·min-1;平均F为44.46%。结论:23-乙酰泽泻醇B在大鼠体内吸收缓慢但较完全

消除相对较快。说明23-乙酰泽泻醇B具有良好的药代动力学特征

便于开发成临床使用方便的药物。

Abstract

Objective: To study the pharmacokinetic and bioavailability of 23-acetyl alisol B from Rhizoma Alismatis by different administration.Method: 23-acetyl alisol B was given by oral administration and intravenous injection to rats respectively and blood sample were withdrawn at different time.23-acetyl alisol B in plasma samples were determined by HPLC-UV method.The mobile phase consisted of acetonitrile and water（80∶20）.The detection wavelength was at 210 nm;the flow rate was 1.0 mL·min-1.The model of pharmacokinetic was built by the drug-time curve and the parameters and absolute bioavailability were calculated.Result: The main pharmacokinetic parameters of 23-acetyl alisol B in rats were Tmax =（122.15 ± 15.23） min

Cmax =（9.89 ± 0.87） mg·L-1

t1/2 =（58.72 ± 6.23） min

AUC0-t =（1 854.970 ± 142.31） mg.min·L-1

AUC0-∞ =（1 875.81 ±144.27） mg.min·L-1

CL /F =（2.89 ± 0.13） mL·min-1 for oral administration and are Tmax =（10.04 ± 0.78）min

Cmax =（42.59 ± 3.47） mg·L-1

t1/2 =（32.05 ± 2.53） min

AUC0-t =（2 810.08 ± 178.70） mg.min·L-1

AUC0-∞ =（2 812.41 ± 224.63） mg.min·L-1

CL /F =（1.74 ± 0.54） mL.min-1 for intravenous injection.Mean bioavailability（F） was 44.46%.Conclustion: The absorption of 23-acetyl alisol B in rats is slow but complete comparing with the quick elimination.It implied that 23-acetyl alisol B has good pharmacokinetic characteristics

and can be easy to develop into a clinical drug which can be convenient to use.

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