首页> 美国卫生研究院文献>Neoplasia (New York N.Y.) >ICI 182780-Regulated Gene Expression in DU145 Prostate Cancer Cells Is Mediated by Estrogen Receptor-β/NFκB Crosstalk
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ICI 182780-Regulated Gene Expression in DU145 Prostate Cancer Cells Is Mediated by Estrogen Receptor-β/NFκB Crosstalk

机译:ICI 182780调控的DU145前列腺癌细胞中的基因表达是由雌激素受体-β/NFκB串扰介导的。

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摘要

Estrogen receptor (ER)-β is the predominant ER subtype in prostate cancer (PCa). We previously demonstrated that ICI 182,780 (ICI), but not estrogens, exerted dose-dependent growth inhibition on DU145 PCa cells by an ER-β-mediated pathway. Transcriptional profiling detected a greater than three-fold upregulation of seven genes after a 12-hour exposure to 1 µM ICI. Semi-quantitative reverse transcriptase polymerase chain reaction confirmed the upregulation of four genes by ICI: interleukin-12α chain, interleukin-8, embryonic growth/differentiation factor, and RYK tyrosine kinase. Treatment with an ER-β antisense oligonucleotide reduced cellular ER-β mRNA and induced loss of expression of these genes. Sequence analysis revealed the presence of consensus NFκB sites, but not estrogen-responsive elements, in promoters of all four genes. Reporter assay and chromatin immunoprecipitation experiments demonstrated that ICI-induced gene expression could be mediated by crosstalk between ER-α and the NFκB signaling pathway, denoting a novel mechanism of ER-β-mediated ICI action. Therefore, combined therapies targeting ER-β and NFκB signaling may be synergistic as treatment for PCa.
机译:雌激素受体(ER)-β是前列腺癌(PCa)中主要的ER亚型。我们先前证明,ICI 182,780(ICI)而非雌激素通过ER-β介导的途径对DU145 PCa细胞发挥剂量依赖性的生长抑制作用。在暴露于1 µM ICI 12小时后,转录谱分析检测到七个基因的上调程度大于三倍。半定量逆转录酶聚合酶链反应证实了ICI对四个基因的上调:白介素12α链,白介素8,胚胎生长/分化因子和RYK酪氨酸激酶。用ER-β反义寡核苷酸处理降低了细胞ER-βmRNA并诱导了这些基因表达的丧失。序列分析显示,在所有四个基因的启动子中均存在共有的NFκB位点,但没有雌激素反应性元件。记者分析和染色质免疫沉淀实验表明,ICI诱导的基因表达可以通过ER-α与NFκB信号通路之间的串扰来介导,这表明ER-β介导的ICI作用的新机制。因此,靶向ER-β和NFκB信号传导的联合疗法可以协同治疗PCa。

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