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CYP7B1相关类固醇对不同细胞系中雄激素受体激活的影响。

Effects of CYP7B1-related steroids on androgen receptor activation in different cell lines.

作者信息

Lundqvist Johan, Norlin Maria

机构信息

Department of Pharmaceutical Biosciences, Box 591, Uppsala University, SE-751 24 Uppsala, Sweden.

出版信息

Biochim Biophys Acta. 2012 Jul;1821(7):973-9. doi: 10.1016/j.bbalip.2012.03.007. Epub 2012 Mar 28.

DOI:10.1016/j.bbalip.2012.03.007
PMID:22484622
Abstract

The widely expressed steroid hydroxylase CYP7B1 is involved in metabolism of a number of steroids reported to influence estrogen and androgen signaling. Several studies by us and other investigators have linked this enzyme to effects on estrogen receptor activation. In a previous report we examined the effect of CYP7B1-mediated hormone metabolism for estrogen-mediated response in kidney-derived HEK293 cells. In the current study we used an androgen response element (ARE) reporter system to examine androgen-dependent response of some CYP7B1 substrates and CYP7B1-formed metabolites in several cell lines derived from different tissues. The results indicate significantly lower androgen receptor activation by CYP7B1-formed steroid metabolites than by the corresponding steroid substrates, suggesting that CYP7B1-mediated catalysis may decrease some androgenic responses. Thus, CYP7B1-dependent metabolism may be of importance not only for estrogenic signaling but also for androgenic. This finding, that CYP7B1 activity may be a regulator of androgenic signaling by converting AR ligands into less active metabolites, is also supported by real-time RT-PCR experiment where a CYP7B1 substrate, but not the corresponding product, was able to stimulate known androgen-sensitive genes. Furthermore, our data indicate that the effects of some steroids on hormone response element reporter systems are cell line-specific. For instance, despite transfection of the same reporter systems, 5-androstene-3β,17β-diol strongly activates an androgen-dependent response element in prostate cancer cells whereas it elicits only ER-dependent responses in kidney HEK293 cells. Potential roles of cell-specific metabolism or comodulator expression for the observed differences are discussed.

摘要

广泛表达的类固醇羟化酶CYP7B1参与了许多据报道会影响雌激素和雄激素信号传导的类固醇的代谢。我们和其他研究人员的多项研究已将这种酶与雌激素受体激活的影响联系起来。在之前的一份报告中,我们研究了CYP7B1介导的激素代谢对肾源性HEK293细胞中雌激素介导反应的影响。在当前的研究中,我们使用雄激素反应元件(ARE)报告系统来检测几种来自不同组织的细胞系中一些CYP7B1底物和CYP7B1形成的代谢产物的雄激素依赖性反应。结果表明,CYP7B1形成的类固醇代谢产物对雄激素受体的激活作用明显低于相应的类固醇底物,这表明CYP7B1介导的催化作用可能会降低一些雄激素反应。因此,CYP7B1依赖性代谢可能不仅对雌激素信号传导很重要,对雄激素信号传导也很重要。这一发现,即CYP7B1活性可能通过将AR配体转化为活性较低的代谢产物来调节雄激素信号传导,也得到了实时RT-PCR实验的支持,在该实验中,一种CYP7B1底物能够刺激已知的雄激素敏感基因,而相应的产物则不能。此外,我们的数据表明,一些类固醇对激素反应元件报告系统的影响具有细胞系特异性。例如,尽管转染了相同的报告系统,但5-雄烯-3β,17β-二醇在前列腺癌细胞中强烈激活雄激素依赖性反应元件,而在肾HEK293细胞中仅引发雌激素依赖性反应。文中还讨论了细胞特异性代谢或共调节因子表达对观察到的差异的潜在作用。

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