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尽管细胞周围蛋白水解活性增加,但LRP-1沉默仍可阻止恶性细胞侵袭。

LRP-1 silencing prevents malignant cell invasion despite increased pericellular proteolytic activities.

作者信息

Dedieu Stéphane, Langlois Benoît, Devy Jérôme, Sid Brice, Henriet Patrick, Sartelet Hervé, Bellon Georges, Emonard Hervé, Martiny Laurent

机构信息

CNRS UMR MEOyC 6237, Laboratoire SiRMA (Signalisation des Récepteurs Matriciels), Université de Reims Champagne-Ardenne, Moulin de la Housse, BP 1039, 51687 Reims Cedex 2, France.

出版信息

Mol Cell Biol. 2008 May;28(9):2980-95. doi: 10.1128/MCB.02238-07. Epub 2008 Mar 3.

Abstract

The scavenger receptor low-density lipoprotein receptor-related protein 1 (LRP-1) mediates the clearance of a variety of biological molecules from the pericellular environment, including proteinases which degrade the extracellular matrix in cancer progression. However, its accurate functions remain poorly explored and highly controversial. Here we show that LRP-1 silencing by RNA interference results in a drastic inhibition of cell invasion despite a strong stimulation of pericellular matrix metalloproteinase 2 and urokinase-type plasminogen activator proteolytic activities. Cell migration in both two and three dimensions is decreased by LRP-1 silencing. LRP-1-silenced carcinoma cells, which are characterized by major cytoskeleton rearrangements, display atypical overspread morphology with a lack of membrane extensions. LRP-1 silencing accelerates cell attachment, inhibits cell-substrate deadhesion, and induces the accumulation, at the cell periphery, of abundant talin-containing focal adhesion complexes deprived of FAK and paxillin. We conclude that in addition to its role in ligand binding and endocytosis, LRP-1 regulates cytoskeletal organization and adhesive complex turnover in malignant cells by modulating the focal complex composition, thereby promoting invasion.

摘要

清道夫受体低密度脂蛋白受体相关蛋白1(LRP - 1)介导从细胞周围环境清除多种生物分子,包括在癌症进展过程中降解细胞外基质的蛋白酶。然而,其确切功能仍未得到充分探索且极具争议性。在此我们表明,尽管细胞周围基质金属蛋白酶2和尿激酶型纤溶酶原激活物的蛋白水解活性受到强烈刺激,但通过RNA干扰使LRP - 1沉默会导致细胞侵袭受到显著抑制。LRP - 1沉默会降低二维和三维空间中的细胞迁移。以主要细胞骨架重排为特征的LRP - 1沉默癌细胞表现出非典型的铺展形态,缺乏膜延伸。LRP - 1沉默加速细胞附着,抑制细胞与底物的解离,并在细胞周边诱导大量富含踝蛋白的粘着斑复合物积累,这些复合物缺乏粘着斑激酶和桩蛋白。我们得出结论,除了其在配体结合和内吞作用中的作用外,LRP - 1还通过调节粘着斑复合物的组成来调节恶性细胞中的细胞骨架组织和粘着复合物更新,从而促进侵袭。

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