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首页> 外文期刊>In vivo. >Regional cyclin D1 overexpression or hypoxia correlate inversely with heterogeneous oestrogen receptor-alpha expression in human breast cancer.
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Regional cyclin D1 overexpression or hypoxia correlate inversely with heterogeneous oestrogen receptor-alpha expression in human breast cancer.

机译:区域细胞周期蛋白D1过表达或缺氧与人乳腺癌中异质雌激素受体-α表达成反比。

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摘要

The oestrogen receptor-alpha (ER alpha) differs in expression and regulation in breast cancer and, by studying the co-factor cyclin D1 as well as changes in the microenvironment, we here delineate two conditions that potentially cause regional down-regulation of the receptor. Heterogeneously expressed ER alpha was observed in 24 out of 134 of the studied breast cancer samples. In 6 out of 24 of the heterogeneous tumours, there was a clear inverse association between cyclin D1 protein/gene amplification and presence of ER alpha. In a subset of 120 tumours, analysed by Western blotting and ELISA, we further showed disparity in differentiation grade and proliferation between tumours with varied cyclin D1/ER alpha content. In another fraction (9 out of 24) of the heterogeneous tumours, there was an inverse association between the ER alpha and Hypoxia-Inducible Factor-1 alpha (HIF-1 alpha) suggesting that ER alpha was down-regulated during hypoxic conditions. These results were verified by culturing ER alpha breast cancer cell lines under hypoxic conditions showing a prominent down-regulation of the ER alpha. The two factors linked to ER alpha down-regulation can also be used to design new treatment approaches interfering with key proteins in these ER alpha regulatory pathways, thereby hopefully increasing the effect of anti-hormonal treatment.
机译:雌激素受体-α(ER alpha)在乳腺癌中的表达和调控有所不同,通过研究辅助因子细胞周期蛋白D1和微环境的变化,我们在此描述了可能导致受体局部下调的两种情况。在研究的134个乳腺癌样品中,有24个观察到异质表达的ERα。在24种异源性肿瘤中,有6种在细胞周期蛋白D1蛋白/基因扩增与ERα的存在之间存在明显的负相关。通过蛋白质印迹和ELISA分析,在120个肿瘤的子集中,我们进一步显示了不同细胞周期蛋白D1 / ERα含量的肿瘤在分化程度和增殖方面的差异。在异质性肿瘤的另一部分(24个中的9个)中,ERα和缺氧诱导因子1α(HIF-1α)之间存在负相关关系,这表明ERα在低氧条件下被下调。这些结果通过在低氧条件下培养ERα乳腺癌细胞系进行了验证,这些细胞系显示出ERα的显着下调。与ERα下调相关的两个因素也可以用于设计新的治疗方法,以干扰这些ERα调节途径中的关键蛋白,从而有望提高抗激素治疗的效果。

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