首页> 美国卫生研究院文献>Journal of the Boston Society of Medical Sciences >Down-Regulation of the Oncogene Cyclin D1 Increases Migratory Capacity in Breast Cancer and Is Linked to Unfavorable Prognostic Features
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Down-Regulation of the Oncogene Cyclin D1 Increases Migratory Capacity in Breast Cancer and Is Linked to Unfavorable Prognostic Features

机译:癌基因细胞周期蛋白D1的下调增加了乳腺癌的迁移能力并与不良的预后特征相关

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摘要

The oncogene cyclin D1 is highly expressed in many breast cancers and, despite its proliferation-activating properties, it has been linked to a less malignant phenotype. To clarify this observation, we focused on two key components of malignant behavior, migration and proliferation, and observed that quiescent G0/G1 cells display an increased migratory capacity compared to cycling cells. We also found that the down-regulation of cyclin D1 in actively cycling cells significantly increased migration while also decreasing proliferation. When analyzing a large set of premenopausal breast cancers, we observed an inverse proliferation-independent link between cyclin D1 and tumor size and recurrence, suggesting that this protein might abrogate infiltrative malignant behavior >in vivo. Finally, gene expression analysis after cyclin D1 down-regulation by siRNA confirmed changes in processes associated with migration and enrichment of our gene set in a metastatic poor prognosis signature. This novel function of cyclin D1 illustrates the interplay between tumor proliferation and migration and may explain the attenuation of malignant behavior in breast cancers with high cyclin D1 levels.
机译:癌基因细胞周期蛋白D1在许多乳腺癌中高表达,尽管具有增殖激活特性,但它与恶性程度较低的表型有关。为了阐明这一发现,我们集中于恶性行为的两个关键组成部分,迁移和增殖,并观察到静态G0 / G1细胞与循环细胞相比显示出更高的迁移能力。我们还发现主动循环细胞中细胞周期蛋白D1的下调显着增加了迁移,同时也降低了增殖。当分析大量绝经前乳腺癌时,我们观察到细胞周期蛋白D1与肿瘤大小和复发之间存在与增殖无关的逆向联系,表明该蛋白可能会消除>体内浸润性恶性行为。最后,通过siRNA下调细胞周期蛋白D1后的基因表达分析证实,与转移和预后不良的基因集富集相关的过程发生了变化。细胞周期蛋白D1的这一新功能说明了肿瘤增殖与迁移之间的相互作用,并可能解释了细胞周期蛋白D1水平高的乳腺癌恶性行为的减弱。

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