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人体药物吸收动力学及其与Caco-2单层通透性的比较。

Human drug absorption kinetics and comparison to Caco-2 monolayer permeabilities.

作者信息

Polli J E, Ginski M J

机构信息

School of Pharmacy, University of Maryland, Baltimore 21201, USA.

出版信息

Pharm Res. 1998 Jan;15(1):47-52. doi: 10.1023/a:1011992518592.

DOI:10.1023/a:1011992518592
PMID:9487545
Abstract

PURPOSE

This study aims to assess the drug absorption kinetics of three drugs and compare their resulting first-order intestinal permeation rate constants to their Caco-2 monolayer permeabilities.

METHODS

In vitro dissolution--in vivo absorption analysis was conducted on four formulations of each ranitidine HCl, metoprolol tartrate, and piroxicam to yield apparent and "true" human clinical permeation rate constants. Drug permeability coefficients through Caco-2 monolayers were also determined.

RESULTS

In vitro dissolution--in vivo absorption analysis revealed different relative and absolute contributions of dissolution and intestinal permeation to overall drug absorption kinetics for various drug formulations and yielded estimates of each drug's true and apparent human intestinal permeation rate constant [kp = 0.225 hr-1, 0.609 hr-1, and 9.00 hr-1 for ranitidine, metoprolol, and piroxicam, respectively]. A rank order relationship was observed for both the apparent and true permeation rate constant with Caco-2 monolayer permeability. The decrease in the true permeation rate constant relative to the apparent permeation rate constant was most significant (almost three-fold) for the least permeable compound, ranitidine.

CONCLUSIONS

There were marked differences in the permeation kinetics of ranitidine, metoprolol, and piroxicam. The possibility of an association between absorption kinetics from dosage forms in humans and Caco-2 monolayer permeability may allow for a direct kinetic interpretation of human oral absorption from Caco-2 monolayer permeability values.

摘要

目的

本研究旨在评估三种药物的药物吸收动力学,并将其所得的一级肠道渗透速率常数与其在Caco-2单层中的渗透率进行比较。

方法

对每种盐酸雷尼替丁、酒石酸美托洛尔和吡罗昔康的四种制剂进行体外溶出-体内吸收分析,以得出表观和“真实”的人体临床渗透速率常数。还测定了药物通过Caco-2单层的渗透系数。

结果

体外溶出-体内吸收分析揭示了不同药物制剂的溶出和肠道渗透对整体药物吸收动力学的相对和绝对贡献不同,并得出了每种药物真实和表观的人体肠道渗透速率常数估计值[雷尼替丁、美托洛尔和吡罗昔康的kp分别为0.225小时-1、0.609小时-1和9.00小时-1]。观察到表观和真实渗透速率常数与Caco-2单层渗透率之间存在等级关系。对于渗透性最低的化合物雷尼替丁,真实渗透速率常数相对于表观渗透速率常数的降低最为显著(几乎三倍)。

结论

雷尼替丁、美托洛尔和吡罗昔康的渗透动力学存在显著差异。人体剂型吸收动力学与Caco-2单层渗透率之间存在关联的可能性,可能允许根据Caco-2单层渗透率值对人体口服吸收进行直接的动力学解释。

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