首页> 外文期刊>Journal of Cell Science >Blocking beta-catenin binding to the ZBP1 promoter represses ZBP1 expression, leading to increased proliferation and migration of metastatic breast-cancer cells.
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Blocking beta-catenin binding to the ZBP1 promoter represses ZBP1 expression, leading to increased proliferation and migration of metastatic breast-cancer cells.

机译:阻止β-catenin与ZBP1启动子的结合会抑制ZBP1表达,从而导致转移性乳腺癌细胞的增殖和迁移增加。

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摘要

ZBP1 (zipcode-binding protein 1, also known as IMP-1) is an mRNA regulator, functioning in mRNA localization, stability and translational control. ZBP1 is actively expressed during embryogenesis and tumorigenesis, but its expression is repressed in metastatic breast-cancer cell lines and tumors. In this article, we show that downregulation of ZBP1 expression results from its promoter methylation, an epigenetic process that remodels the chromatin structure and frequently represses gene activity. Demethylation of the ZBP1 promoter in metastatic cells reactivated ZBP1 expression, owing to restoration of the interaction of the ZBP1 promoter with beta-catenin. Loss of ZBP1 function not only increased growth ability of metastatic cells, but also promoted cell migration. We identified a number of mRNAs that were selectively associated with ZBP1 in breast-cancer cells. Many of these are involved in cell motility and in cell-cycle regulation, and displayed altered expression patterns in the absence of ZBP1. These data suggest that repression of ZBP1 deregulates its associated mRNAs, leading to the phenotypic changes of breast cancers.
机译:ZBP1(邮政编码结合蛋白1,也称为IMP-1)是一种mRNA调节剂,在mRNA定位,稳定性和翻译控制中起作用。 ZBP1在胚胎发生和肿瘤发生过程中活跃表达,但在转移性乳腺癌细胞系和肿瘤中其表达受到抑制。在本文中,我们显示ZBP1表达的下调是由其启动子甲基化导致的,该基因是一个重塑染色质结构并经常抑制基因活性的表观遗传过程。由于恢复了ZBP1启动子与β-catenin的相互作用,转移细胞中ZBP1启动子的去甲基化重新激活了ZBP1表达。 ZBP1功能的丧失不仅增加了转移细胞的生长能力,而且促进了细胞迁移。我们鉴定了一些与乳腺癌细胞中ZBP1选择性相关的mRNA。其中许多涉及细胞运动性和细胞周期调控,并且在不存在ZBP1的情况下表现出改变的表达模式。这些数据表明,ZBP1的阻遏调节其相关的mRNA,从而导致乳腺癌的表型改变。

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