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首页> 外文期刊>Neoplasia: an international journal for oncology research >NRF2 Mutation Confers Malignant Potential and Resistance to Chemoradiation Therapy in Advanced Esophageal Squamous Cancer
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NRF2 Mutation Confers Malignant Potential and Resistance to Chemoradiation Therapy in Advanced Esophageal Squamous Cancer

机译:NRF2突变在晚期食管鳞癌中赋予恶性潜力和抗化学疗法治疗

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摘要

Esophageal squamous cancer (ESC) is one of the most aggressive tumors of the gastrointestinal tract. A combination of chemotherapy and radiation therapy (CRT) has improved the clinical outcome, but the molecular background determining the effectiveness of therapy remains unknown. NRF2 is a master transcriptional regulator of stress adaptation, and gain of-function mutation of NRF2 in cancer confers resistance to stressors including anticancer therapy. Direct resequencing analysis revealed that Nrf2 gain-of-function mutation occurred recurrently (18/82, 22%) in advanced ESC tumors and ESC cell lines (3/10). The presence of Nrf2 mutation was associated with tumor recurrence and poor prognosis. Short hairpin RNA-mediated down-regulation of NRF2 in ESC cells that harbor only mutated Nrf2 allele revealed that themutant NRF2 conferred increased cell proliferation, attachment-independent survival, and resistance to 5-fluorouracil and γ-irradiation. Based on the Nrf2 mutation status, gene expression signatures associated with NRF2 mutation were extracted from ESC cell lines, and their potential utility for monitoring and prognosis was examined in a cohort of 33 pre-CRT cases of ESC. The molecular signatures of NRF2 mutation were significantly predictive and prognostic for CRT response. In conclusion, recurrent NRF2 mutation confers malignant potential and resistance to therapy in advanced ESC, resulting in a poorer outcome. Molecular signatures of NRF2 mutation can be applied as predictive markers of response to CRT, and efficient inhibition of aberrant NRF2 activation could be a promising approach in combination with CRT.
机译:食管鳞癌(ESC)是胃肠道最具侵袭性的肿瘤之一。化疗和放射治疗(CRT)的组合改善了临床结果,但确定治疗的有效性的分子背景仍然未知。 NRF2是癌症适应的主转录调节器,癌症中NRF2的功能突变突变赋予抗癌治疗等压力源的抗性。直接重试分析显示,在高级ESC肿瘤和ESC细胞系(3/10)中,NRF2常用(18/82,22%)发生常用(18/82,22%)。 NRF2突变的存在与肿瘤复发和预后不良有关。短发夹RNA介导的NRF2在ESC细胞中的下调仅突变NRF2等位基因显示,小组NRF2赋予增加的细胞增殖,附着的依赖性存活率和抗5氟尿嘧啶和γ-辐照。基于NRF2突变状态,从ESC细胞系提取与NRF2突变相关的基因表达签名,并在ESC的33个CRT病例的队列中检查它们的监测和预后的潜在效用。 NRF2突变的分子鉴定对于CRT反应显着预测和预后。总之,复发性NRF2突变赋予高级ESC中恶性潜力和对治疗的抵抗力,导致较差的结果。 NRF2突变的分子鉴定可以作为对CRT的响应的预测标志物应用,并且有效抑制异常NRF2活化可以是与CRT组合的有希望的方法。

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