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Inhibition of hypoxia-induced miR-155 radiosensitizes hypoxic lung cancer cells

机译:抑制低氧诱导的miR-155放射增敏低氧性肺癌细胞

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摘要

miR-155 is a prominent microRNA (miRNA) that regulates genes involved in immunity and cancer-related pathways. miR-155 is overexpressed in lung cancer, which correlates with poor patient prognosis. It is unclear how miR-155 becomes increased in lung cancers and how this increase contributes to reduced patient survival. Here, we show that hypoxic conditions induce miR-155 expression in lung cancer cells and trigger a corresponding decrease in a validated target, FOXO3A. Furthermore, we find that increased levels of miR-155 radioprotects lung cancer cells, while inhibition of miR-155 radiosensitizes these cells. Moreover, we reveal a therapeutically important link between miR-155 expression, hypoxia, and irradiation by demonstrating that anti-miR-155 molecules also sensitize hypoxic lung cancer cells to irradiation. Our study helps explain how miR-155 becomes elevated in lung cancers, which contain extensive hypoxic microenvironments, and demonstrates that inhibition of miR-155 may have important therapeutic potential as a means to radiosensitize hypoxic lung cancer cells.
机译:miR-155是一种杰出的microRNA(miRNA),可调节涉及免疫力和癌症相关途径的基因。 miR-155在肺癌中过表达,与患者预后不良相关。尚不清楚miR-155在肺癌中如何增加以及这种增加如何导致患者生存期缩短。在这里,我们显示低氧条件诱导肺癌细胞中miR-155的表达,并触发经过验证的靶标FOXO3A相应降低。此外,我们发现增加水平的miR-155可以保护肺癌细胞,而抑制miR-155可以使这些细胞敏感。此外,我们通过证明抗miR-155分子也使低氧性肺癌细胞对辐射敏感,从而揭示了miR-155表达,缺氧和辐射之间的重要治疗联系。我们的研究有助于解释miR-155在含有大量低氧微环境的肺癌中如何升高,并证明抑制miR-155可能具有重要的治疗潜力,可作为对低氧肺癌细胞进行放射增敏的手段。

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