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Integrins synergise to induce expression of the MRTF-A-SRF target gene ISG15 for promoting cancer cell invasion

机译:整合素协同诱导MRTF-A-SRF靶基因ISG15的表达以促进癌细胞侵袭

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Integrin-mediated activation of small GTPases induces the polymerisation of G-actin into various actin structures and the release of the transcriptional co-activator MRTF from G-actin. Here we report that pan-integrin-null fibroblasts seeded on fibronectin and expressing beta 1- and/or alpha V-class integrin contained different G-actin pools, nuclear MRTF-A (also known as MKL1 or MAL) levels and MRTF-A-SRF activities. The nuclear MRTF-A levels and activities were highest in cells expressing both integrin classes, lower in cells expressing beta 1 integrins and lowest in cells expressing the alpha V integrins. Quantitative proteomics and transcriptomics analyses linked the differential MRTF-A activities to the expression of the ubiquitin-like modifier interferon-stimulated gene 15 (ISG15), which is known to modify focal adhesion and cytoskeletal proteins. The malignant breast cancer cell line MDA-MB-231 expressed high levels of beta 1 integrins, ISG15 and ISGylated proteins, which promoted invasive properties, whereas non-invasive MDA-MB-468 and MCF-7 cell lines expressed low levels of beta 1 integrins, ISG15 and ISGylated proteins. Our findings suggest that integrin-adhesion-induced MRTF-A-SRF activation and ISG15 expression constitute a newly discovered signalling circuit that promotes cell migration and invasion.
机译:整联蛋白介导的小GTP酶的激活诱导G-肌动蛋白聚合成各种肌动蛋白结构,并从G-肌动蛋白释放转录共激活因子MRTF。在这里我们报告说,泛整联蛋白无效的成纤维细胞接种在纤连蛋白上并表达β1和/或αV类整联蛋白包含不同的G-肌动蛋白池,核MRTF-A(也称为MKL1或MAL)水平和MRTF-A -SRF活动。在表达两种整联蛋白类型的细胞中,核MRTF-A水平和活性最高,在表达β1整联蛋白的细胞中较低,而在表达αV整联蛋白的细胞中最低。定量蛋白质组学和转录组学分析将不同的MRTF-A活性与泛素样修饰剂干扰素刺激基因15(ISG15)的表达联系起来,该基因已知可以改变粘着斑和细胞骨架蛋白。恶性乳腺癌细胞系MDA-MB-231表达高水平的β1整联蛋白,ISG15和ISGylated蛋白,从而促进了侵袭性,而非侵袭性MDA-MB-468和MCF-7细胞系表达了低水平的β1整合素,ISG15和ISGylated蛋白。我们的发现表明,整联蛋白粘附诱导的MRTF-A-SRF激活和ISG15表达构成了新发现的促进细胞迁移和侵袭的信号传导电路。

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