首页> 外文期刊>Neoplasma: Journal of Experimental and Clinical Oncology >Fn14 receptor promotes invasive potential and metastatic capacity of non-small lung adenocarcinoma cells through the up-regulation of integrin alpha 6
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Fn14 receptor promotes invasive potential and metastatic capacity of non-small lung adenocarcinoma cells through the up-regulation of integrin alpha 6

机译:Fn14受体通过上调整合素α6促进非小肺腺癌细胞的侵袭潜能和转移能力

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摘要

Lung cancer is one of the leading cause of cancer-related death around the world with the majority of diagnoses being non-small cell lung cancer (NSCLC). Given the poor survival rate and efficacy of current therapy for NSCLC, there is a need to identify and develop new therapeutic targets for treatment. We have observed significantly up-regulated levels of Fn14 in clinical samples of lung cancer relative to normal adjacent tissue. However, the functional role of Fn14 in these tumors is not understood yet. We used RT-PCR to establish the Fn14 expression profile in various NSCLC cell lines. Using isogenic variants of H460 NSCLC cell line with low, intermediate and high Fn14 expression as a cellular model, we determined that increased levels of integrin alpha 6 in cells over-expressing Fn14 is suggestive of an important role of alpha 6 beta 1-fn14 interactions in motility of lung carcinoma and formation of metastases. Enhanced levels of Fn14 correlated with higher tumor cell migration and invasion in an MMP-1 dependent manner. Cells over-expressing Fn14 showed increased in vivo tumor formation with metastatic capacity to lymph nodes, lungs and liver. Thus, this research maybe a step toward developing improved treatment strategies for NSCLC by improved detection and inhibition of metastases.
机译:肺癌是世界范围内与癌症相关的死亡的主要原因之一,多数诊断为非小细胞肺癌(NSCLC)。鉴于目前非小细胞肺癌的生存率和疗效较差,有必要确定和开发新的治疗靶标。我们已经观察到相对于正常的相邻组织,肺癌临床样品中Fn14的水平明显上调。然而,Fn14在这些肿瘤中的功能作用尚不清楚。我们使用RT-PCR在各种NSCLC细胞系中建立Fn14表达谱。使用具有低,中和高Fn14表达的H460 NSCLC细胞系的同基因变体作为细胞模型,我们确定过表达Fn14的细胞中整联蛋白alpha 6的水平升高暗示了alpha 6 beta 1-fn14相互作用的重要作用在肺癌的运动和转移的形成。 Fn14的水平升高与更高的肿瘤细胞迁移和侵袭相关,且呈MMP-1依赖性。过度表达Fn14的细胞显示体内肿瘤形成增加,并具有转移至淋巴结,肺和肝的能力。因此,这项研究可能是通过改善转移的检测和抑制,为NSCLC发展改善的治疗策略迈出的一步。

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