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在怀孕小鼠中,肝 Cyp2d 和 Cyp26a1 的 mRNA 和活性增加。

Hepatic Cyp2d and Cyp26a1 mRNAs and activities are increased during mouse pregnancy.

机构信息

School of Pharmacy, Department of Pharmaceutics, University of Washington, Seattle, WA 98195-7610, USA.

出版信息

Drug Metab Dispos. 2013 Feb;41(2):312-9. doi: 10.1124/dmd.112.049379. Epub 2012 Nov 13.

Abstract

There is considerable evidence that drug disposition is altered during human pregnancy and based on probe drug studies, CYP2D6 activity increases during human pregnancy. The aim of this study was to determine whether the changes of CYP2D6 activity observed during human pregnancy could be replicated in the mouse, and explore possible mechanisms of increased CYP2D6 activity during pregnancy. Cyp2d11, Cyp2d22, Cyp2d26 and Cyp2d40 mRNA was increased (P < 0.05) on gestational days (GD) 15 and 19 compared with the non-pregnant controls. There was no change (P > 0.05) in Cyp2d9 and Cyp2d10 mRNA. In agreement with the increased Cyp2d mRNA, Cyp2d-mediated dextrorphan formation from dextromethorphan was increased 2.7-fold (P < 0.05) on GD19 (56.8±39.4 pmol/min/mg protein) when compared with the non-pregnant controls (20.8±11.2 pmol/min/mg protein). An increase in Cyp26a1 mRNA (10-fold) and retinoic acid receptor (Rar)β mRNA (2.8-fold) was also observed during pregnancy. The increase in Cyp26a1 and Rarβ mRNA during pregnancy indicates increased retinoic acid signaling in the liver during pregnancy. A putative retinoic acid response element was identified within the Cyp2d40 promoter and the mRNA of Cyp2d40 correlated (P < 0.05) with Cyp26a1 and Rarβ. These results show that Cyp2d mRNA is increased during mouse pregnancy the and mouse may provide a suitable model to investigate the mechanisms underlying the increased clearance of CYP2D6 probes observed during human pregnancy. Our findings also suggest that retinoic acid signaling in the liver is increased during pregnancy, which may have broader implications to energy homeostasis in the liver during pregnancy.

摘要

有大量证据表明,药物处置在人类妊娠期间发生改变,并且基于探针药物研究,CYP2D6 活性在人类妊娠期间增加。本研究的目的是确定在人类妊娠期间观察到的 CYP2D6 活性变化是否可以在小鼠中复制,并探索妊娠期间 CYP2D6 活性增加的可能机制。与非妊娠对照组相比,Cyp2d11、Cyp2d22、Cyp2d26 和 Cyp2d40mRNA 在妊娠第 15 天和第 19 天增加(P < 0.05)。Cyp2d9 和 Cyp2d10mRNA 没有变化(P > 0.05)。与 Cyp2d mRNA 的增加一致,与非妊娠对照组(20.8±11.2 pmol/min/mg 蛋白)相比,Cyp2d 介导的右美沙芬从右美沙芬形成的右美沙芬增加了 2.7 倍(P < 0.05)在妊娠第 19 天(56.8±39.4 pmol/min/mg 蛋白)。在妊娠期间还观察到 Cyp26a1mRNA(10 倍)和视黄酸受体(Rar)βmRNA(2.8 倍)的增加。妊娠期间 Cyp26a1 和 RarβmRNA 的增加表明妊娠期间肝脏中的视黄酸信号增加。在 Cyp2d40 启动子内鉴定出推定的视黄酸反应元件,并且 Cyp2d40mRNA 与 Cyp26a1 和 Rarβ相关(P < 0.05)。这些结果表明,在小鼠妊娠期间 Cyp2dmRNA 增加,并且小鼠可能提供合适的模型来研究在人类妊娠期间观察到的 CYP2D6 探针清除增加的机制。我们的发现还表明,妊娠期间肝脏中的视黄酸信号增加,这可能对妊娠期间肝脏的能量稳态产生更广泛的影响。

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