Radiation Oncology Branch, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, Maryland.
Department of Radiology and Imaging Sciences, Clinical Center, National Institutes of Health, Bethesda, Maryland.
Mol Cancer Ther. 2018 Feb;17(2):355-367. doi: 10.1158/1535-7163.MCT-17-0262. Epub 2017 Aug 11.
Implementing targeted drug therapy in radio-oncologic treatment regimens has greatly improved the outcome of cancer patients. However, the efficacy of molecular targeted drugs such as inhibitory antibodies or small molecule inhibitors essentially depends on target expression and activity, which both can change during the course of treatment. Radiotherapy has previously been shown to activate prosurvival pathways, which can help tumor cells to adapt and thereby survive treatment. Therefore, we aimed to identify changes in signaling induced by radiation and evaluate the potential of targeting these changes with small molecules to increase the therapeutic efficacy on cancer cell survival. Analysis of "The Cancer Genome Atlas" database disclosed a significant overexpression of , and genes in human prostate cancer samples compared with normal prostate gland tissue. Multifractionated radiation of three-dimensional-cultured prostate cancer cell lines with a dose of 2 Gy/day as a clinically relevant schedule resulted in an increased protein phosphorylation and enhanced protein-protein interaction between AKT and mTOR, whereas gene expression of , and related kinases was not altered by radiation. Similar results were found in a xenograft model of prostate cancer. Pharmacologic inhibition of mTOR/AKT signaling after activation by multifractionated radiation was more effective than treatment prior to radiotherapy. Taken together, our findings provide a proof-of-concept that targeting signaling molecules after activation by radiotherapy may be a novel and promising treatment strategy for cancers treated with multifractionated radiation regimens such as prostate cancer to increase the sensitivity of tumor cells to molecular targeted drugs.
在放射肿瘤治疗方案中实施靶向药物治疗极大地改善了癌症患者的预后。然而,分子靶向药物(如抑制性抗体或小分子抑制剂)的疗效本质上取决于靶标表达和活性,而这两者在治疗过程中都会发生变化。放疗先前已被证明能激活促生存途径,这有助于肿瘤细胞适应并从而存活下来。因此,我们旨在确定辐射诱导的信号变化,并评估用小分子靶向这些变化以提高癌症细胞存活的治疗效果的潜力。“癌症基因组图谱”数据库的分析显示,与正常前列腺组织相比,人类前列腺癌样本中 、 和 基因的表达显著上调。每天 2 Gy 的三维培养前列腺癌细胞系进行多分次照射,是一种临床相关的方案,导致 AKT 和 mTOR 之间的蛋白磷酸化增加和蛋白-蛋白相互作用增强,而辐射对 、 和相关激酶的基因表达没有改变。在前列腺癌的异种移植模型中也发现了类似的结果。在多分次照射激活后,抑制 mTOR/AKT 信号通路比在放疗前治疗更有效。总之,我们的研究结果提供了一个概念验证,即针对放疗激活后的信号分子进行靶向治疗可能是一种新的有前途的治疗策略,可用于治疗多分次放疗方案(如前列腺癌),以提高肿瘤细胞对分子靶向药物的敏感性。