AKT 活性水平高与对 MEK 抑制剂 AZD6244(ARRY-142886)的耐药性有关。
High level of AKT activity is associated with resistance to MEK inhibitor AZD6244 (ARRY-142886).
机构信息
Department of Thoracic and Cardiovascular Surgery, The University of Texas M.D. Anderson Cancer Center, Houston, TX, USA.
出版信息
Cancer Biol Ther. 2009 Nov;8(21):2073-80. doi: 10.4161/cbt.8.21.9844. Epub 2009 Nov 18.
Abstract
MEK/ERK activities are increased in many primary lung cancers, and MEK inhibitors have been tested clinically for treatment of non-small cell lung cancers. The molecular mechanisms of resistance to MEK inhibitors have not been clearly demonstrated, however, and no molecular biomarker that can predict lung cancer response to MEK inhibitors is available. By determining the dose-responses of 35 human lung cancer cell lines to MEK-specific inhibitor AZD6244, we identified subsets of lung cancer cell lines that are either sensitive or resistant to this agent. Subsequent molecular characterization showed that treatment with AZD6244 suppressed ERK phosphorylation in both sensitive and resistant cells, suggesting that resistance is not mediated by the activities of MEK/ERK themselves. Interestingly, we found that levels of phosphorylated AKT were dramatically higher in the resistant cancer cells than in the sensitive cells. Stable transfection of dominant-negative AKT into resistant cells by retroviral infection restored their susceptibility to AZD6244. These results indicate that phosphorylated AKT may be a biomarker of response to AZD6244 and that modulation of AKT activity may be a useful approach to overcome resistance to MEK inhibitors.
摘要
MEK/ERK 活性在许多原发性肺癌中增加,并且已经在临床上测试了 MEK 抑制剂用于治疗非小细胞肺癌。然而,对 MEK 抑制剂的耐药性的分子机制尚未得到明确证实,也没有可预测肺癌对 MEK 抑制剂反应的分子生物标志物。通过确定 35 个人类肺癌细胞系对 MEK 特异性抑制剂 AZD6244 的剂量反应,我们鉴定了对该药物敏感或耐药的肺癌细胞系亚群。随后的分子特征分析表明,AZD6244 处理抑制了敏感和耐药细胞中 ERK 的磷酸化,表明耐药性不是由 MEK/ERK 本身的活性介导的。有趣的是,我们发现耐药癌细胞中磷酸化 AKT 的水平明显高于敏感细胞。通过逆转录病毒感染将显性失活 AKT 稳定转染入耐药细胞中,恢复了它们对 AZD6244 的敏感性。这些结果表明,磷酸化 AKT 可能是对 AZD6244 反应的生物标志物,并且调节 AKT 活性可能是克服 MEK 抑制剂耐药性的有用方法。
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