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Strong fascin expression promotes metastasis independent of its F-actin bundling activity

机译:fascin的强表达促进转移而与其F-actin捆绑活性无关

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摘要

High expression of the actin bundling protein Fascin increases the malignancy of tumor cells. Here we show that fascin expression is up-regulated in more malignant sub-cell lines of MDA-MB-231 cells as compared to parental cells. Since also parental MDA-MB-231 cells exhibit high fascin levels, increased fascin expression was termed as “hyperexpression”. To examine the effect of fascin hyperexpression, fascin was hyperexpressed in parental MDA-MB-231 cells and metastasis was analyzed in NOD scid gamma (NSG) mice. In addition, the effect of fascin mutants with inactive or constitutively active actin bundling activity was examined. Unexpectedly, we found that hyperexpression of both, wildtype (wt) and mutant fascin strongly increased metastasis in vivo, showing that the effect of fascin hyperexpression did not depend on its actin bundling activity. Cellular assays revealed that hyperexpression of wt and mutant fascin increased adhesion of MDA-MB-231 cells while transmigration and proliferation were not affected. Since it has been shown that fascin controls adhesion by directly interacting with microtubules (MTs), we analyzed if fascin hyperexpression affects MT dynamics. We found that at high concentrations fascin significantly increased MT dynamics in cells and in cell-free approaches. In summary our data show that strong expression of fascin in breast cancer cells increases metastasis independent of its actin bundling activity. Thus, it seems that the mechanism of fascin-stimulated metastasis depends on its concentration.
机译:肌动蛋白捆绑蛋白Fascin的高表达增加了肿瘤细胞的恶性程度。在这里我们显示,与亲代细胞相比,fascin表达在MDA-MB-231细胞的更多恶性亚细胞系中上调。由于亲本的MDA-MB-231细胞也表现出高的fascin水平,因此增加的fascin表达被称为“过表达”。为了检查fascin高表达的作用,在亲代MDA-MB-231细胞中fascin高表达,并在NOD scidγ(NSG)小鼠中分析了转移。此外,检查了具有非活性或组成性肌动蛋白束缚活性的fascin突变体的作用。出乎意料的是,我们发现野生型(wt)和突变型fascin的过表达都大大增加了体内转移,表明fascin过表达的作用并不取决于其肌动蛋白束缚活性。细胞分析表明,wt和突变型fascin的过表达增加了MDA-MB-231细胞的粘附性,而迁移和增殖均未受到影响。由于已经证明fascin通过直接与微管(MT)相互作用来控制粘附,因此我们分析了fascin的过表达是否影响MT动力学。我们发现,在高浓度下,fascin会显着增加细胞和无细胞方法中MT的动力学。总而言之,我们的数据表明,fascin在乳腺癌细胞中的强表达增加了转移,而与肌动蛋白的束缚活性无关。因此,似乎fascin刺激转移的机制取决于其浓度。

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