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首页> 外文期刊>British Journal of Cancer >ATP7A is a novel target of retinoic acid receptor |[beta]|2 in neuroblastoma cells
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ATP7A is a novel target of retinoic acid receptor |[beta]|2 in neuroblastoma cells

机译:ATP7A是神经母细胞瘤细胞中视黄酸受体|β| 2的新靶标

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Increased retinoic acid receptor β (RARβ2) gene expression is a hallmark of cancer cell responsiveness to retinoid anticancer effects. Moreover, low basal or induced RARβ2 expression is a common feature of many human cancers, suggesting that RARβ2 may act as a tumour suppressor gene in the absence of supplemented retinoid. We have previously shown that low RARβ2 expression is a feature of advanced neuroblastoma. Here, we demonstrate that the ABC domain of the RARβ2 protein alone was sufficient for the growth inhibitory effects of RARβ2 on neuroblastoma cells. ATP7A, the copper efflux pump, is a retinoid-responsive gene, was upregulated by ectopic overexpression of RARβ2. The ectopic overexpression of the RARβ2 ABC domain was sufficient to induce ATP7A expression, whereas, RARβ2 siRNA blocked the induction of ATP7A expression in retinoid-treated neuroblastoma cells. Forced downregulation of ATP7A reduced copper efflux and increased viability of retinoid-treated neuroblastoma cells. Copper supplementation enhanced cell growth and reduced retinoid-responsiveness, whereas copper chelation reduced the viability and proliferative capacity. Taken together, our data demonstrates ATP7A expression is regulated by retinoic acid receptor β and it has effects on intracellular copper levels, revealing a link between the anticancer action of retinoids and copper metabolism.
机译:维甲酸受体β(RARβ2)基因表达的增加是癌细胞对类维生素A抗癌作用的反应的标志。而且,低的基础或诱导的RARβ2表达是许多人类癌症的共同特征,表明RARβ2可以在缺乏补充类维生素A的情况下充当肿瘤抑制基因。先前我们已经表明,RARβ2低表达是晚期神经母细胞瘤的特征。在这里,我们证明了单独的RARβ2蛋白的ABC域足以满足RARβ2对神经母细胞瘤细胞的生长抑制作用。铜外排泵ATP7A是类维生素A响应基因,由于异位RARβ2过表达而被上调。 RARβ2ABC结构域的异位过表达足以诱导ATP7A表达,而RARβ2siRNA阻断了类维生素A处理的神经母细胞瘤细胞中ATP7A表达的诱导。 ATP7A的强制下调减少了铜的外排并增加了类维生素A处理的神经母细胞瘤细胞的活力。补充铜可促进细胞生长,并降低类维生素A的反应性,而铜螯合则可降低活力和增殖能力。两者合计,我们的数据表明ATP7A的表达受视黄酸受体β的调节,并且对细胞内铜水平有影响,揭示了类维生素A的抗癌作用与铜代谢之间的联系。

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