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首页> 美国卫生研究院文献>other >Cancer Associated Fibroblast-Derived Hepatocyte Growth Factor Inhibits the Paclitaxel-Induced Apoptosis of Lung Cancer A549 Cells by Up-Regulating the PI3K/Akt and GRP78 Signaling on a Microfluidic Platform
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Cancer Associated Fibroblast-Derived Hepatocyte Growth Factor Inhibits the Paclitaxel-Induced Apoptosis of Lung Cancer A549 Cells by Up-Regulating the PI3K/Akt and GRP78 Signaling on a Microfluidic Platform

机译:癌症相关的成纤维细胞衍生的肝细胞生长因子通过上调微流体平台上的PI3K / Akt和GRP78信号传导抑制紫杉醇诱导的肺癌A549细胞凋亡。

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Tumor stroma and growth factors provide a survival environment to tumor cells and can modulate their chemoresistance by dysregulating several signal pathways. In this study, we fabricated a three-dimensional (3D) microfluidic chip using polydimethylsiloxane (PDMS) to investigate the impact of hepatocyte growth factor (HGF) from cancer-associated fibroblasts (CAF) on the Met/PI3K/AKT activation, glucose regulatory protein (GRP78) expression and the paclitaxel-induced A549 cell apoptosis. With a concentration gradient generator, the assembled chip was able to reconstruct a tumor microenvironment in vitro. We found high levels of HGF in the supernatants of CAF and the CAF matrix from the supernatants of activated HFL1 fibroblasts or HGF enhanced the levels of Met, PI3K and AKT phosphorylation and GRP78 expression in A549 cells cultured in a 3D cell chamber, which was abrogated by anti-HGF. Inhibition of Met attenuated the CAF matrix-enhanced PI3K/AKT phosphorylation and GRP78 expression while inhibition of PI3K reduced GRP78 expression, but not Met phosphorylation in A549 cells. Inhibition of GRP78 failed to modulate the CAF matrix-enhanced Met/PI3K/AKT phosphorylation in A549 cells. Furthermore, inhibition of PI3K or GRP78 enhanced spontaneous and paclitaxel-induced A549 cell apoptosis. Moreover, treatment with the CAF matrix inhibited spontaneous and medium or high dose of paclitaxel-induced A549 cell apoptosis. Inhibition of PI3K or GRP78 attenuated the CAF matrix-mediated inhibition on paclitaxel-induced A549 cell apoptosis. Our data indicated that HGF in the CAF matrix activated the Met/PI3K/AKT and up-regulated GRP78 expression, promoting chemoresistance to paclitaxel-mediated apoptosis in A549 cells. Our findings suggest that the microfluidic system may represent an ideal platform for signaling research and drug screening.
机译:肿瘤基质和生长因子为肿瘤细胞提供了生存环境,并可以通过失调几种信号通路来调节其化学耐药性。在这项研究中,我们使用聚二甲基硅氧烷(PDMS)制作了三维(3D)微流控芯片,以研究癌症相关成纤维细胞(CAF)的肝细胞生长因子(HGF)对Met / PI3K / AKT活化,葡萄糖调节的影响蛋白(GRP78)表达和紫杉醇诱导的A549细胞凋亡。使用浓度梯度发生器,组装的芯片能够在体外重建肿瘤微环境。我们发现活化的HFL1成纤维细胞上清液中CAF和CAF基质上清液中的高水平HGF或HGF增强了在3D细胞室中培养的A549细胞中的Met,PI3K和AKT磷酸化水平以及GRP78表达的水平通过抗HGF。 Met的抑制作用减弱了CAF基质增强的PI3K / AKT磷酸化和GRP78的表达,而PI3K的抑制作用则降低了A549细胞的GRP78表达,但未抑制Met的磷酸化。 GRP78的抑制未能调节A549细胞中CAF基质增强的Met / PI3K / AKT磷酸化。此外,PI3K或GRP78的抑制作用增强了自发和紫杉醇诱导的A549细胞凋亡。而且,用CAF基质处理抑制了紫杉醇诱导的自发性和中剂量或高剂量的紫杉醇诱导的A549细胞凋亡。 PI3K或GRP78的抑制作用减弱了CAF基质介导的对紫杉醇诱导的A549细胞凋亡的抑制作用。我们的数据表明,CAF基质中的HGF激活Met / PI3K / AKT并上调GRP78表达,从而促进对紫杉醇介导的A549细胞凋亡的化学耐药性。我们的发现表明,微流控系统可能代表信号研究和药物筛选的理想平台。

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