药物激活核受体的进化:一个祖先基因在哺乳动物中分化成两个异种传感器基因。

Christoph Handschin, Sharon Blättler, Adrian Roth, Renate Looser, Mikael Oscarson, Michel R Kaufmann, Michael Podvinec, Carmela Gnerre, Urs A Meyer
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引用次数: 38

摘要

背景:在哺乳动物中,药物和其他外源药物通过激活妊娠X受体(PXR)和组成型雄烷受体(CAR)来改变细胞色素P450 (CYP)的基因表达。在非哺乳动物物种中,只发现了一种异种传感器基因。本研究以鸡为模型生物,目的是阐明非哺乳动物物种是否像哺乳动物一样只有一种或两种异种感受器。结果:为了探索这种差异的进化方面,我们试图通过各种实验方法在鸡中识别额外的外源感应核受体。然而,这些都没有发现新的候选人。通过RNAi或显性阴性等位基因消融鸡外源性受体(CXR)功能可显著降低鸡肝癌细胞系的药物诱导。随后,我们对CXR进行了功能和结构表征,并将我们的结果与PXR和CAR进行了比较。尽管它们的氨基酸序列高度相似,但PXR和CAR具有非常不同的激活模式。CXR功能的一些方面,如直接配体激活和高混杂性,很容易让人联想到PXR。另一方面,细胞定位研究揭示了CXR和CAR在细胞质-核分布方面的共同特征。最后,与PXR和CAR相比,CXR在调节方面具有独特的特性。结论:我们的发现有力地表明,在哺乳动物中,CXR构成了一个进化成PXR和CAR的祖先基因。未来的研究应该阐明哺乳动物与非哺乳动物物种之间这种差异的原因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The evolution of drug-activated nuclear receptors: one ancestral gene diverged into two xenosensor genes in mammals.

The evolution of drug-activated nuclear receptors: one ancestral gene diverged into two xenosensor genes in mammals.

The evolution of drug-activated nuclear receptors: one ancestral gene diverged into two xenosensor genes in mammals.

The evolution of drug-activated nuclear receptors: one ancestral gene diverged into two xenosensor genes in mammals.

BACKGROUND: Drugs and other xenobiotics alter gene expression of cytochromes P450 (CYP) by activating the pregnane X receptor (PXR) and constitutive androstane receptor (CAR) in mammals. In non-mammalian species, only one xenosensor gene has been found. Using chicken as a model organism, the aim of our study was to elucidate whether non-mammalian species only have one or two xenosensors like mammals. RESULTS: To explore the evolutionary aspect of this divergence, we tried to identify additional xenobiotic sensing nuclear receptors in chicken using various experimental approaches. However, none of those revealed novel candidates. Ablation of chicken xenobiotic receptor (CXR) function by RNAi or dominant-negative alleles drastically reduced drug-induction in a chicken hepatoma cell line. Subsequently, we functionally and structurally characterized CXR and compared our results to PXR and CAR. Despite the high similarity in their amino acid sequence, PXR and CAR have very distinct modes of activation. Some aspects of CXR function, e.g. direct ligand activation and high promiscuity are very reminiscent of PXR. On the other hand, cellular localization studies revealed common characteristics of CXR and CAR in terms of cytoplasmic-nuclear distribution. Finally, CXR has unique properties regarding its regulation in comparison to PXR and CAR. CONCLUSION: Our finding thus strongly suggest that CXR constitutes an ancestral gene which has evolved into PXR and CAR in mammals. Future studies should elucidate the reason for this divergence in mammalian versus non-mammalian species.

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