Steroid-induced epithelial-fibroblastic conversion associated with syndecan suppression in S115 mouse mammary tumor cells.

Cell regulation Pub Date : 1991-01-01 DOI:10.1091/mbc.2.1.1
S Leppä, P Härkönen, M Jalkanen
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引用次数: 66

Abstract

Cell-matrix interactions play an important role in the maintenance of cell shape, supposed to be mediated by the anchorage of cellular cytoskeleton to extracellular matrix via matrix receptors. In this work the expression of one of the known matrix receptors, syndecan, was studied during the hormone-induced change in the phenotype of Shionogi 115 (S115) mouse mammary tumor cells. In the presence of testosterone, when S115 cells express fibroblastic phenotype, they increased their growth rate and became gradually anchorage independent. These cells, however, revealed strong RGDS-dependent binding to fibronectin (FN) but not binding to the heparin-binding domain of FN. Instead, S115 cells growth without testosterone showed epithelial morphology and binding to the heparin-binding domain of FN, suggesting an alteration of syndecan expression in hormone-treated S115 cells. As quantitated by radioimmunoassay and by Western blot, the amounts of both matrix-binding ectodomain of syndecan and syndecan mRNA (2.6 kb) declined in hormone-treated S115 cells. The addition of antiandrogen cyproterone acetate to culture medium opposed the effect of testosterone on syndecan mRNA. We thus propose that the inactivation of syndecan gene and the consequent suppression of syndecan expression is related to the altered adhesion properties, the disappearance of epithelial phenotype, and, on the other hand, to the appearance of transformed-like phenotype in hormone-treated S115 cells.

类固醇诱导的上皮-成纤维细胞转化与S115小鼠乳腺肿瘤细胞的syndecan抑制相关。
细胞-基质相互作用在维持细胞形状中起着重要作用,细胞骨架通过基质受体锚定在细胞外基质上。在这项工作中,我们研究了一种已知基质受体syndecan在激素诱导的Shionogi 115 (S115)小鼠乳腺肿瘤细胞表型变化过程中的表达。在睾酮存在的情况下,当S115细胞表达成纤维细胞表型时,它们的生长速度加快,并逐渐变得锚定独立。然而,这些细胞显示出与纤维连接蛋白(FN)强烈的rgds依赖性结合,而不与FN的肝素结合结构域结合。相反,在没有睾酮的情况下,S115细胞的生长表现出上皮形态,并与FN的肝素结合结构域结合,这表明激素处理的S115细胞中syndecan的表达发生了变化。通过放射免疫分析和Western blot定量分析,激素处理的S115细胞中syndecan和syndecan mRNA (2.6 kb)的基质结合外结构域数量均下降。在培养基中添加抗雄激素醋酸环丙孕酮与睾酮对syndecan mRNA的影响相反。因此,我们提出syndecan基因的失活以及由此导致的syndecan表达的抑制与激素处理的S115细胞粘附特性的改变、上皮表型的消失,以及另一方面与转化样表型的出现有关。
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