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Periostin suppression induces decorin secretion leading to reduced breast cancer cell motility and invasion

机译:骨膜素抑制诱导除芯蛋白分泌,导致乳腺癌细胞运动和侵袭减少

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The ability of cancer cells to metastasize is dependent on the interactions between their cell-surface molecules and the microenvironment. However, the tumor microenvironment, especially the cancer-associated stroma, is poorly understood. To identify proteins present in the stroma, we focused on phyllodes tumors, rare breast tumors that contain breast stromal cells. We compared the expression of proteins between phyllodes tumor and normal tissues using an iTRAQ-based quantitative proteomic approach. Decorin was expressed at reduced levels in phyllodes tumor tissues, whereas periostin was upregulated; this result was validated by immunohistochemical analysis of phyllodes tumors from 35 patients. Additionally, by immunoprecipitation and mass spectrometry, we confirmed that decorin forms a complex with periostin in both phyllodes tumors and BT-20 breast cancer cells. Following siRNA-mediated knockdown of periostin in T-47D cells, secreted decorin in the culture medium could be detected by multiple reaction monitoring (MRM). Furthermore, periostin knockdown in BT-20 cells and overexpression of decorin in MDA-MB-231 cells inhibited cell motility and invasion. Our results reveal the molecular details of the periostin–decorin complex in both phyllodes tumor tissues and breast cancer cells; this interaction may represent a novel target for anti-cancer therapy.
机译:癌细胞转移的能力取决于其细胞表面分子与微环境之间的相互作用。然而,人们对肿瘤的微环境,尤其是与癌症相关的基质的了解却很少。为了鉴定基质中存在的蛋白质,我们集中研究了叶状肿瘤,这是一种含有乳腺基质细胞的罕见乳腺肿瘤。我们使用基于iTRAQ的定量蛋白质组学方法比较了叶状体肿瘤和正常组织之间蛋白质的表达。 Decorin在叶状肿瘤组织中表达降低,而骨膜素上调。免疫组化分析了35例患者的叶状肿瘤,证实了这一结果。此外,通过免疫沉淀和质谱法,我们确认了得体蛋白在叶状体肿瘤和BT-20乳腺癌细胞中均与骨膜素形成复合物。在siRNA介导的T-47D细胞中骨膜素的敲低之后,可以通过多反应监测(MRM)检测培养基中分泌的核心蛋白聚糖。此外,BT-20细胞中的骨膜素抑制和MDA-MB-231细胞中的得体蛋白的过表达抑制了细胞运动和侵袭。我们的研究结果揭示了叶状肿瘤组织和乳腺癌细胞中骨膜素-decorin复合物的分子细节。这种相互作用可能代表了抗癌治疗的新目标。

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