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Ascites-induced shift along epithelial-mesenchymal spectrum in ovarian cancer cells: Enhancement of their invasive behavior partly dependant on αv integrins

机译:腹水诱导卵巢癌细胞沿上皮-间充质谱转移:侵袭行为的增强部分取决于αv整合素

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At least one-third of patients with epithelial ovarian cancer (OC) present ascites at diagnosis and almost all have ascites at recurrence. The presence of ascites, which acts as a dynamic reservoir of active molecules and cellular components, correlates with the OC peritoneal metastasis and is associated with poor prognosis. Since epithelial-mesenchymal transition (EMT) is involved in different phases of OC progression, we have investigated the effect of the unique ascitic tumor microenvironment on the EMT status and the behavior of OC cells. The exposure of three OC cell lines to ascites leads to changes in cellular morphologies. Within ascites, OC cells harboring an initial intermediate epithelial phenotype are characterized by marked dislocation of epithelial markers (E-cadherin, ZO-1 staining) while OC cells initially harboring an intermediate mesenchymal phenotype strengthen their mesenchymal markers (N-cadherin, vimentin). Ascites differentially triggers a dissemination phenotype related to the initial cell features by either allowing the proliferation and the formation of spheroids and the extension of colonies for cells that present an initial epithelial intermediate phenotype, or favoring the migration of cells with a mesenchymal intermediate phenotype. In an ascitic microenvironment, a redeployment of αv integrins into cells was observed and the ascites-induced accentuation of the two different invasive phenotypes (i.e. spheroids formation or migration) was shown to involve αv integrins. Thus, ascites induces a shift toward an unstable intermediate state of the epithelial-mesenchymal spectrum and confers a more aggressive cell behavior that takes on a different pathway based on the initial epithelial-mesenchymal cell features.
机译:至少有三分之一的上皮性卵巢癌(OC)患者在诊断时出现腹水,几乎所有患者在复发时都有腹水。腹水的存在,可作为活性分子和细胞成分的动态储存库,与OC腹膜转移有关,并与预后不良有关。由于上皮-间质转化(EMT)参与OC进展的不同阶段,我们已经研究了独特的腹水肿瘤微环境对EMT状态和OC细胞行为的影响。三种OC细胞系暴露于腹水会导致细胞形态发生变化。在腹水中,具有初始中间上皮表型的OC细胞的特征在于上皮标记物的明显脱位(E-钙粘着蛋白,ZO-1染色),而最初具有中间间质表型的OC细胞则增强了它们的间充质标记(N-钙粘着蛋白,波形蛋白)。腹水通过允许呈初始上皮中间表型的细胞增殖和形成球体并扩展菌落,或促进具有间充质中间表型的细胞的迁移,从而差异性地触发与初始细胞特征相关的扩散表型。在一个腹水微环境中,观察到αv整联蛋白重新部署到细胞中,并且显示腹水诱导的两种不同侵入性表型(即球体形成或迁移)的突触涉及αv整联蛋白。因此,腹水诱导上皮-间充质光谱向不稳定的中间状态转变,并赋予了更具侵略性的细胞行为,该行为基于初始的上皮-间充质细胞特征采取了不同的途径。

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