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妊娠对小鼠细胞色素P450 3a和P-糖蛋白表达及活性的影响:机制、组织特异性和时间进程

Effect of pregnancy on cytochrome P450 3a and P-glycoprotein expression and activity in the mouse: mechanisms, tissue specificity, and time course.

作者信息

Zhang Huixia, Wu Xiaohui, Wang Honggang, Mikheev Andrei M, Mao Qingcheng, Unadkat Jashvant D

机构信息

Department of Pharmaceutics, University of Washington, Seattle, WA 98195, USA.

出版信息

Mol Pharmacol. 2008 Sep;74(3):714-23. doi: 10.1124/mol.107.043851. Epub 2008 May 28.

Abstract

The plasma concentrations of orally administered anti-human immunodeficiency virus protease inhibitors are significantly reduced during human and mouse pregnancy. We have shown that in the mouse, at gestational day 19, this reduction is due to increased hepatic cytochrome P450 3a (Cyp3a) protein expression and activity. In the current study, we investigated the mechanisms by which Cyp3a activity is increased by pregnancy and the time course of change in expression of Cyp3a and P-glycoprotein (P-gp) in various tissues. We found that hepatic transcripts of Cyp3a16, Cyp3a41, and Cyp3a44 were significantly increased during pregnancy, whereas those of Cyp3a11 and Cyp3a25 were significantly decreased. This resulted in a net increase in Cyp3a protein expression and activity in the liver during pregnancy. The increase in Cyp3a41 and Cyp3a44 transcripts was positively correlated (p < 0.05) with hepatocyte nuclear factor 6 and estrogen receptor-alpha transcripts. The pregnancy-related factors that transcriptionally activated mouse Cyp3a isoforms also activated the human CYP3A4 promoter in pregnant CYP3A4-promoter-luciferase transgenic (CYP3A4-tg) mice. In contrast, intestinal Cyp3a protein expression was not significantly affected by pregnancy. No change in P-gp protein expression was observed in the liver or kidney during pregnancy, although a significant decrease was observed in the placenta. Because hepatic CYP3A activity also seems to be induced during human pregnancy, the mouse (including CYP3A4-tg mouse) seems to be an excellent animal model to determine the molecular mechanisms for such an induction.

摘要

口服抗人类免疫缺陷病毒蛋白酶抑制剂的血浆浓度在人类和小鼠妊娠期间会显著降低。我们已经表明,在小鼠妊娠第19天时,这种降低是由于肝脏细胞色素P450 3a(Cyp3a)蛋白表达和活性增加所致。在当前研究中,我们调查了妊娠导致Cyp3a活性增加的机制以及不同组织中Cyp3a和P-糖蛋白(P-gp)表达变化的时间进程。我们发现,妊娠期间Cyp3a16、Cyp3a41和Cyp3a44的肝脏转录本显著增加,而Cyp3a11和Cyp3a25的转录本则显著减少。这导致妊娠期间肝脏中Cyp3a蛋白表达和活性净增加。Cyp3a41和Cyp3a44转录本的增加与肝细胞核因子6和雌激素受体α转录本呈正相关(p < 0.05)。转录激活小鼠Cyp3a亚型的妊娠相关因子也激活了妊娠CYP3A4启动子荧光素酶转基因(CYP3A4-tg)小鼠中的人类CYP3A4启动子。相比之下,肠道Cyp3a蛋白表达不受妊娠的显著影响。妊娠期间肝脏或肾脏中未观察到P-gp蛋白表达的变化,尽管在胎盘中观察到显著下降。由于人类妊娠期间肝脏CYP3A活性似乎也被诱导,小鼠(包括CYP3A4-tg小鼠)似乎是确定这种诱导分子机制的理想动物模型。

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