索拉非尼抑制结直肠癌细胞中 p38α 的活性,并与 DFG-in 抑制剂 SB202190 协同作用,增加细胞凋亡反应。
Sorafenib inhibits p38α activity in colorectal cancer cells and synergizes with the DFG-in inhibitor SB202190 to increase apoptotic response.
机构信息
Cancer Genetics Laboratory, IRCCS S. de Bellis, Castellana Grotte, Italy.
出版信息
Cancer Biol Ther. 2012 Dec;13(14):1471-81. doi: 10.4161/cbt.22254. Epub 2012 Sep 17.
Abstract
In the search for new strategies to efficiently fight colorectal cancer, efforts are being increasingly focused on targeting regulatory signaling pathways involved in cancer-specific features. As a result, several studies have recently addressed the therapeutic potential of molecularly-targeted drugs capable of inhibiting the activity of protein kinases involved in relevant signaling cascades. Here we show that simultaneous inhibition of the DFG-in and DFG-out conformations of p38α by means of type-I and type-II inhibitors is beneficial to impair more efficiently its kinase activity. Moreover, we found that SB202190 (type-I) and sorafenib (type-II) synergize at the molecular and biological level, as co-treatment with these compounds enhances tumor growth inhibition and induction of apoptosis both in colorectal cancer cell lines and animal models. These results support the need to reconsider sorafenib as a therapeutic agent against colorectal cancer and provide new insights that underline the importance to elucidate the activity of protein kinase inhibitors for the treatment of colorectal carcinoma.
摘要
在寻找有效对抗结直肠癌的新策略时,人们越来越关注靶向参与癌症特异性特征的调节信号通路。因此,最近有几项研究探讨了能够抑制相关信号级联中蛋白激酶活性的分子靶向药物的治疗潜力。在这里,我们表明通过使用 I 型和 II 型抑制剂同时抑制 p38α 的 DFG-in 和 DFG-out 构象,有利于更有效地削弱其激酶活性。此外,我们发现 SB202190(I 型)和索拉非尼(II 型)在分子和生物学水平上具有协同作用,因为这些化合物的联合治疗增强了结直肠癌细胞系和动物模型中的肿瘤生长抑制和凋亡诱导。这些结果支持重新考虑索拉非尼作为治疗结直肠癌的药物的必要性,并提供了新的见解,强调了阐明蛋白激酶抑制剂活性用于治疗结直肠癌的重要性。
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