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通过基质抑制同时估算肝脏内在清除率和蛋白结合率的新方法。

New method for the simultaneous estimation of intrinsic hepatic clearance and protein binding by matrix inhibition.

作者信息

Uchimura Takahide, Kato Motohiro, Tachibana Tatsuhiko, Arai Shinichi, Nabuchi Yoshiaki, Saito Kimitoshi, Kinoshita Haruki

机构信息

Fuji Gotemba Research Laboratories, Chugai Pharmaceutical Co. Ltd, Gotemba, Shizuoka, Japan.

出版信息

Biopharm Drug Dispos. 2008 Jan;29(1):7-16. doi: 10.1002/bdd.583.

Abstract

The purpose of this study was to develop a method for estimating the hepatic clearance (CL(h)) without using a protein binding test. This method allows the simultaneous evaluation of the intrinsic hepatic clearance (CL(int)) with a correction for microsomal binding, and the free fraction in the serum (fu). It uses the decrease in metabolic velocity achieved by decreasing the free fraction of a compound in the incubation mixture (fu(inc)) by the addition of serum, and by changing the microsomal protein concentration. This method is denoted as the 'matrix inhibition method', because it uses the inhibition of the metabolic velocity by the incubation matrix. The metabolic rates of eight compounds (diazepam, imipramine, warfarin, and compounds A-E) were evaluated under several incubation conditions using rat serum and microsomes. The correlation of CL(int) evaluated using the method and using equilibrium dialysis after the CL(int) was corrected for microsomal binding was r = 0.968. The correlation of fu . CL(int) was r = 0.996. Although the method required a high enough fu and fu(microsomes) difference among the reaction conditions for each compound, it could evaluate CL(int) and fu simultaneously and easily by adding additional reaction conditions to the metabolic stability tests performed in ADME screening.

摘要

本研究的目的是开发一种无需进行蛋白结合试验即可估算肝清除率(CL(h))的方法。该方法能够在对微粒体结合进行校正的同时评估内在肝清除率(CL(int))以及血清中的游离分数(fu)。它利用通过添加血清降低孵育混合物中化合物的游离分数(fu(inc))以及改变微粒体蛋白浓度所导致的代谢速度降低。此方法被称为“基质抑制法”,因为它利用了孵育基质对代谢速度的抑制作用。使用大鼠血清和微粒体在几种孵育条件下评估了八种化合物(地西泮、丙咪嗪、华法林以及化合物A - E)的代谢率。在对CL(int)进行微粒体结合校正后,使用该方法评估的CL(int)与使用平衡透析评估的CL(int)之间的相关性为r = 0.968。fu·CL(int)的相关性为r = 0.996。尽管该方法要求每种化合物在反应条件之间有足够大的fu和fu(微粒体)差异,但通过在ADME筛选中进行的代谢稳定性试验增加额外的反应条件,它能够同时且轻松地评估CL(int)和fu。

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