MK-2206,一种 Akt 抑制剂,增强了胃癌细胞系中卡铂/紫杉醇的疗效。
MK-2206, an Akt inhibitor, enhances carboplatinum/paclitaxel efficacy in gastric cancer cell lines.
机构信息
H. Lee Moffitt Cancer Center & Research Institute; Tampa, FL USA.
出版信息
Cancer Biol Ther. 2013 Oct 1;14(10):932-6. doi: 10.4161/cbt.25939. Epub 2013 Aug 5.
BACKGROUND
Several molecularly-targeted agents are being evaluated in gastric cancer cell lines. In this study we evaluated the synergistic potential of MK-2206, an oral potent allosteric Akt inhibitor, in combination with chemotherapeutic agents in human gastric cancer cell lines.
MATERIALS AND METHODS
We evaluated effects of MK-2206 on cell growth and cell signaling using a panel of gastric cancer cell lines AGS, SNU-1 and SNU 16. The analysis of drug combinations was conducted by using CellTiter-Blue™ Cell Viability Assay which yielded the combination index (CI). MK-2206 and representative chemotherapy agent were further evaluated regarding their effects on Akt inhibition and downstream targets using western blots probed with the appropriate antibodies. We assessed the combination of MK-2206 and chemotherapy in three different treatment sequences.
RESULTS
We demonstrated in vitro synergistic efficacy of MK-2206 when combined with carboplatinum and paclitaxel in the three cell lines examined. Efficacy was dose dependent. We assessed the combination of MK-2206 and carboplatinum/paclitaxel in three different treatment sequences; 24 h of exposure to combination chemotherapy followed by a 48 h exposure to MK-2206 resulted in the highest synergistic antiproliferative effect in all cell lines. On the other hand, the reverse sequence (MK-2206 followed by chemotherapy) and the concurrent treatment schedule were slightly synergistic or additive as well. The effects of MK-2206 on p-Akt and other downstream targets was reported.
CONCLUSIONS
Our findings suggest that Akt inhibition augments the efficacy of existing gastric cancer therapeutics (carboplatinum and paclitaxel); thus, MK-2206 is a promising agent to treat gastric cancer patients who receive these cytotoxic agents. The magnitude of synergy depended on the treatment sequence; a schedule of MK-2206 dosed before or concurrently with chemotherapy was not as effective as being dosed after chemotherapy. Further experiments addressing MK-2206's mechanism of action in combination with chemotherapy are needed.
背景
目前有多种针对特定分子靶点的药物正在进行胃癌细胞系的研究。在本研究中,我们评估了口服强效变构 Akt 抑制剂 MK-2206 与化疗药物联合应用于人类胃癌细胞系的协同潜力。
材料与方法
我们使用AGS、SNU-1 和 SNU 16 三种胃癌细胞系,通过细胞增殖试验和细胞信号通路分析,评估了 MK-2206 对细胞生长和细胞信号的影响。采用 CellTiter-Blue™ 细胞活力检测试剂盒分析药物联合作用,得到了组合指数(CI)。进一步采用 Western blot 检测合适的抗体,分析 MK-2206 与代表性化疗药物联合应用对 Akt 抑制及其下游靶点的影响。我们评估了三种不同的治疗顺序下 MK-2206 与化疗药物联合应用的效果。
结果
我们在三种细胞系中均证实了 MK-2206 与卡铂和紫杉醇联合应用具有体外协同疗效。疗效与剂量相关。我们评估了三种不同的治疗顺序下 MK-2206 与卡铂/紫杉醇联合应用的效果;24 小时联合化疗后再暴露于 MK-2206 48 小时,在所有细胞系中均产生了最高的协同抗增殖作用。另一方面,相反的顺序(MK-2206 先于化疗)和同时治疗方案也具有轻微的协同或相加作用。我们还报道了 MK-2206 对 p-Akt 及其他下游靶点的作用。
结论
我们的研究结果表明,Akt 抑制增强了现有胃癌治疗药物(卡铂和紫杉醇)的疗效;因此,MK-2206 是一种有前途的药物,可用于治疗接受这些细胞毒性药物的胃癌患者。协同作用的程度取决于治疗顺序;MK-2206 在化疗前或同时给药的方案不如化疗后给药的方案有效。需要进一步的实验来确定 MK-2206 与化疗联合应用的作用机制。
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