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首页> 外文期刊>OncoTargets and therapy >Transcription factor E2F1 positively regulates interferon regulatory factor 5 expression in non-small cell lung cancer
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Transcription factor E2F1 positively regulates interferon regulatory factor 5 expression in non-small cell lung cancer

机译:转录因子E2F1积极调节非小细胞肺癌中干扰素调节因子5的表达

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摘要

Purpose: Lung cancer is the most common malignant tumor in the world, and its incidence and mortality are very high. This study focuses on the mechanism of non-small cell lung cancer to find new therapeutic targets. Methods: We used RT-PCR and Western blot to verify the linear relationship between E2F1 and IRF5 in normal lung tissue and lung cancer tissues. Secondly, we used overexpression and knock down E2F1 in cell lines to detect the expression of IRF5. The prime enzyme reporter plasmid verified that E2F1 binds to the core promoter region of IRF5; finally, CHIP experiments demonstrated that E2F1 binds directly to IRF5. Results: We verified that E2F1 and IRF5 are decreased in patient tissues, and there is a strong linear relationship between E2F1 and IRF5. Secondly, we used overexpression of E2F1 or E2F1 siRNA transfected into HCC827 cells and found that E2F1 positively regulates the activity of the IRF5 promoter and the mRNA level of IRF5. Finally, the results of a chromatin immunoprecipitation assay demonstrated that E2F1 bound to the promoter region of IRF5 in vitro. These results suggested that the E2F1 transcription factor is the primary determinant for activating the basal transcription of the IRF5. Conclusion: The transcription factor E2F1 positively regulates IRF5 in non-small cell lung cancer.
机译:目的:肺癌是世界上最常见的恶性肿瘤,其发病率和死亡率很高。这项研究着重于非小细胞肺癌寻找新治疗靶点的机制。方法:我们使用RT-PCR和Western blot验证E2F1和IRF5在正常肺组织和肺癌组织中的线性关系。其次,我们使用过表达并敲低细胞系中的E2F1来检测IRF5的表达。初免报告基因质粒证实E2F1与IRF5的核心启动子区结合;最后,CHIP实验证明E2F1直接与IRF5结合。结果:我们证实患者组织中E2F1和IRF5减少,并且E2F1和IRF5之间存在很强的线性关系。其次,我们使用了转染到HCC827细胞中的E2F1或E2F1 siRNA的过表达,发现E2F1正调控IRF5启动子的活性和IRF5的mRNA水平。最后,染色质免疫沉淀试验的结果表明,E2F1在体外与IRF5的启动子区域结合。这些结果表明E2F1转录因子是激活IRF5的基础转录的主要决定因素。结论:转录因子E2F1在非小细胞肺癌中正调控IRF5。

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