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首页> 外文期刊>Cancer Cell International >MicroR-545 enhanced radiosensitivity via suppressing Ku70 expression in Lewis lung carcinoma xenograft model
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MicroR-545 enhanced radiosensitivity via suppressing Ku70 expression in Lewis lung carcinoma xenograft model

机译:通过抑制Lewis肺癌异种移植模型的Ku70表达,MICROR-545通过抑制KU70表达增强放射敏感性

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Radiotherapy is an important therapeutic method for lung cancer. However, in clinical situations, cellular resistance to radiotherapy is a significant component of tumor treatment failure. Thus, clarification in cellular mechanism underlying radiosensitivity of cancer cell is urgently needed. In this study, we established a radiation model of Lewis lung carcinoma in C57BL/6 mice and investigated the possible signaling molecule involved in this process. C57BL/6 mice were subcutaneously transplanted with Lewis lung carcinoma cells and locally irradiated followed by measurement in tumor volume. Levels of miR-545 and Ku70 mRNA expression were determined by using Quantitative Real-Time PCR. Expression of Ku70 was determined by using western blot assay. Cell viability was analyzed by MTT assay. Cell apoptosis was examined by using TUNEL assay. In mice bearing Lewis lung carcinoma tumor, local radiotherapy suppressed tumor growth as well as enhanced expression of miR-545 and downregulated Ku70 level. Inhibition of miR-545 expression reduced radiosensitivity of Lewis tumor. In vitro Lewis lung carcinoma cells experiment, we observed that miR-545 regulated Ku70 expression by targeting Ku70 3′UTR and this process was involved in radiotherapy. This was demonstrated by result of cell proliferation assay in which irradiation reduced apoptosis of cells was mediated by miR-545 inactivation which was reversed by Ku70 silence. miR-545 increased radiosensitivity of Lewis lung carcinoma via inhibiting Ku70 expression.
机译:放射疗法是肺癌的重要治疗方法。然而,在临床局势中,对放射疗法的细胞抗性是肿瘤治疗衰竭的重要组成部分。因此,迫切需要癌细胞隐射性敏感性的细胞机制的澄清。在这项研究中,我们在C57BL / 6小鼠中建立了Lewis肺癌的辐射模型,并研究了该方法中涉及的可能的信号分子。用Lewis肺癌细胞皮下移植C57BL / 6小鼠,然后在肿瘤体积中进行局部照射。通过使用定量实时PCR测定miR-545和Ku70 mRNA表达的水平。通过使用蛋白质印迹测定来确定KU70的表达。通过MTT测定分析细胞活力。通过使用TUNEL测定检查细胞凋亡。在轴承路易斯肺癌肿瘤的小鼠中,局部放射疗法抑制肿瘤生长以及增强miR-545的表达和下调的Ku70水平。 miR-545表达的抑制降低了路易斯肿瘤的放射敏感性。在体外Lewis肺癌细胞实验中,我们观察到MiR-545通过靶向KU70 3'UTR调节KU70表达,并且该过程涉及放射疗法。通过细胞增殖测定结果证明了,其中通过ku70沉默反转的miR-545灭活来介导细胞凋亡的辐射。 MiR-545通过抑制KU70表达增加了Lewis肺癌的放射敏感性。

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