异绿原酸A在大鼠体内的生物利用度和药物代谢动力学

程漩格; 王素军; 曾洁; 钟运鸣; 黄丽花; 臧林泉; 陈吉生

doi:10.13422/j.cnki.syfjx.2015160079

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异绿原酸A在大鼠体内的生物利用度和药物代谢动力学

药物代谢 | 更新时间：2024-01-04

- 异绿原酸A在大鼠体内的生物利用度和药物代谢动力学
- Absolute Bioavailability and Pharmacokinetics of Isochlorogenic Acid A in Rats
- 中国实验方剂学杂志 2015年21卷第16期页码：79-82
- 作者机构：
- 作者简介：
- 基金信息：
  
  国家自然科学基金项目(81073141);广东省“十二五”医学重点学科项目(81073141)
- DOI：10.13422/j.cnki.syfjx.2015160079
  中图分类号： R965
- 纸质出版日期：2015
- 稿件说明：
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程漩格, 王素军, 曾洁, 等. 异绿原酸A在大鼠体内的生物利用度和药物代谢动力学[J]. 中国实验方剂学杂志, 2015,21(16):79-82.

CHENG Xuan-ge, WANG Su-jun, ZENG Jie, et al. Absolute Bioavailability and Pharmacokinetics of Isochlorogenic Acid A in Rats[J]. Chinese journal of experimental traditional medical formulae, 2015, 21(16): 79-82.
程漩格, 王素军, 曾洁, 等. 异绿原酸A在大鼠体内的生物利用度和药物代谢动力学[J]. 中国实验方剂学杂志, 2015,21(16):79-82. DOI： 10.13422/j.cnki.syfjx.2015160079.

CHENG Xuan-ge, WANG Su-jun, ZENG Jie, et al. Absolute Bioavailability and Pharmacokinetics of Isochlorogenic Acid A in Rats[J]. Chinese journal of experimental traditional medical formulae, 2015, 21(16): 79-82. DOI： 10.13422/j.cnki.syfjx.2015160079.

摘要

目的: 研究异绿原酸A在大鼠体内的生物利用度和药代动力学

为该制剂的临床应用提供参考。方法: 建立大鼠血浆中异绿原酸A的HPLC检测

检测波长300 nm

流动相甲醇-0.1%磷酸水(50 :50)。考察大鼠经静脉注射(32 mg ·kg-1)与灌胃(90 mg ·kg-1)给予异绿原酸A后的血药浓度变化

利用3P97软件计算药动学参数

根据药时曲线下面积AUC0-∞和给药剂量

计算异绿原酸A的绝对生物利用度。结果: 异绿原酸A在0.16~110.00 mg ·L-1线性良好(R2=0.998);质量浓度分别为0.43

6.88

55.00 mg ·L-1的异绿原酸A的提取回收率分别为(89.43±2.84)%

(93.16±3.95)%

(85.91±2.04)%;日内精密度RSD分别为11.8%

4.0%

日间精密度RSD分别为6.5%

5.8%

5.8%。大鼠静脉注射和灌胃异绿原酸A后

异绿原酸A在大鼠体内的代谢过程均符合二室模型

消除半衰期分别为(29.49±0.75)

(44.48±0.13) min

AUC0-∞分别为(355.40±32.58)

(319.91±51.00) mg ·min-1 ·L-1。异绿原酸A在大鼠体内的绝对生物利用度30.71%。结论: 异绿原酸A在大鼠体内的过程符合线性动力学过程

且代谢快、半衰期短。

Abstract

Objective: To study pharmacokinetics and bioavailability of isochlorogenic acid A in rats with different adiminstration way. Method: A HPLC method was developed for determination of isochlorogenic acid A in rat plasma.Intravenous and intragastric doses of 32 mg ·kg-1 and 90 mg ·kg-1 were respectively administered

the concentration of isochlorogenic acid A were determined with HPLC

detection wavelength was set at 300 nm.Pharmacokinetic parameters were calculated with 3P97 software.Absolute bioavailability of isochlorogenic acid A was calculated according to AUC0-∞ and doses of isochlorogenic acid A by intravenous and intragastric administration. Result: Excellent linear relationship was obtained in the range of 0.16-110.00 mg ·L-1 with R2 of 0.998.Recoveries of isochlorogenic acid A with three concentrations (0.43

6.88

55.00 mg ·L-1) were (89.43±2.84)%

(93.16±3.95)% and (85.91±2.04)%.The intra-day RSD were 11.8%

4.0% and 4.0%.The inter-day RSD were 6.5%

5.8% and 5.8%

respectively.Metabolic processes of isochlorogenic acid A in rats fitted in with two-compartment model following intravenous and intragastric administration.Elimination half-life were (29.49±0.75) min and (44.48±0.13) min. AUC0-∞ were(355.40±32.58)

(319.91±51.00) mg ·min-1 ·L-1.Its absolute bioavailability in rats was 30.71%. Conclusion: Metabolic processes of isochlorogenic acid A in rats conform to linear dynamics with fast metabolism and short half-life.

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