摘要
目的:探讨酪氨酸蛋白激酶抑制剂盐酸埃克替尼(Icotinib)对人非小细胞肺癌(NSCLC)HCC827细胞Akt通路的活化和凋亡相关蛋白PARP、Caspase-3和Caspase-8表达的影响。方法:将体外培养的人肺癌HCC827细胞分为Icotinib处理组和未处理的对照组,采用四甲基偶氮唑盐法(MTT)检测Icotinib对细胞增殖的抑制作用,采用Western blot检测蛋白表达,应用SPSS 13.0进行统计学分析。结果:Icotinib处理HCC827细胞48h的IC50为0.65μmol/L;选用0.001、0.01μmol/L和0.1μmol/L的Icotinib分别作用HCC827细胞48h,细胞凋亡率分别为(3.35±1.77)%、(8.95±3.18)%和(20.4±3.12)%(P<0.05)。与对照组相比,Icotinib明显抑制Akt的磷酸化水平,诱导PARP、Caspase-3和Caspase-8活化裂解。结论:Icotinib通过抑制Akt信号通路的活化、进一步诱导PARP、Caspase-3和Caspase-8裂解,进而抑制人NSCLC细胞增殖及诱导细胞凋亡。
Objective:To explore the effects of Icotinib on the activation of Akt and the expressions of apoptosis - related proteins in human non - small cell lung cancer cells (NSCLC). Methods: Cell proliferation was measured using MTT assay. The expressions of proteins were detected by Western blot. All experimental data were analyzed with SPSS (13.0 soft). Results: Icotinib significantly inhibited HCC827 cell viability and the eoncertration of inhibited cell viability ( IC50 ) for 48h was 0.65 μmol/L. After treatment with 0. 001,0.01 μmol/L and 0.1 μmol/L Icotinib for 48h, the rates of cell apoptosis were (3.35 ± 1.77 ) %, ( 8.95 ± 3.18 ) % and (20.4 ± 3.12), respectively. Icotinib could upregulated the expression of cleavage of Caspase - 8, Caspase - 3 and PARP. After treated 24 h, Icotinib could obviously decrease the expressions of the phosphorylated Akt in HCC827 cells. Conclusion: Ieotinib inhibited the activation of the Akt signaling pathway, which consequently upregulated the split of the cleavage of Caspase - 8, Caspase -3 and PARP proteins in HCC827 cells.
出处
《现代肿瘤医学》
CAS
2013年第4期686-689,共4页
Journal of Modern Oncology
基金
国家自然科学基金资助项目(No.81172369
81270036)
辽宁省科技厅资助项目(No.2011404013-5)
