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依非韦伦在原代人肝细胞中诱导CYP3A4的作用:与利福平及苯巴比妥的比较

Induction of CYP3A4 by efavirenz in primary human hepatocytes: comparison with rifampin and phenobarbital.

作者信息

Hariparsad Niresh, Nallani Srikanth C, Sane Rucha S, Buckley Donna J, Buckley Arthur R, Desai Pankaj B

机构信息

College of Pharmacy, University of Cincinnati Medical Center, 3223 Eden Avenue, Mail Location #0004, Cincinnati, OH 45267, USA.

出版信息

J Clin Pharmacol. 2004 Nov;44(11):1273-81. doi: 10.1177/0091270004269142.

Abstract

The antiretroviral agent efavirenz enhances the systemic clearance of coadministered drugs that are cytochrome P450 (CYP) 3A4 substrates. The mechanism of the apparent increase in CYP3A4 activity by efavirenz and the magnitude of change relative to other known inducers are not known. The authors tested the hypothesis that increased enzymatic activity by efavirenz entails CYP3A4 induction and activation of the human pregnane X receptor (hPXR), a key transcriptional regulator of CYP3A4. Employing primary cultures of human hepatocytes, they compared the CYP3A4 inductive effects of efavirenz (1-10 microM) to rifampin (10 microM) and phenobarbital (2 mM). A cell-based reporter assay was employed to assess hPXR activation. The authors observed that efavirenz caused a concentration-dependent CYP3A4 induction and hPXR activation. Based on the CYP3A4 activity assay, the average magnitude of induction by efavirenz (5-10 microM) was approximately 3- to 4-fold. In comparison, phenobarbital (2 mM) and rifampin (10 microM) caused a 5- and 6-fold induction, respectively.

摘要

抗逆转录病毒药物依非韦伦可提高同时服用的作为细胞色素P450(CYP)3A4底物的药物的全身清除率。依非韦伦使CYP3A4活性明显增加的机制以及相对于其他已知诱导剂的变化幅度尚不清楚。作者检验了以下假设:依非韦伦增加的酶活性需要CYP3A4诱导以及人孕烷X受体(hPXR)的激活,hPXR是CYP3A4的关键转录调节因子。利用原代人肝细胞培养,他们将依非韦伦(1 - 10微摩尔)与利福平(10微摩尔)和苯巴比妥(2毫摩尔)的CYP3A4诱导作用进行了比较。采用基于细胞的报告基因检测来评估hPXR的激活。作者观察到依非韦伦引起了浓度依赖性的CYP3A4诱导和hPXR激活。基于CYP3A4活性检测,依非韦伦(5 - 10微摩尔)的平均诱导幅度约为3至4倍。相比之下,苯巴比妥(2毫摩尔)和利福平(10微摩尔)分别引起了5倍和6倍的诱导。

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