摘要
目的利用已构建的CCND1表达沉默及过表达的人源性胶质母细胞瘤细胞株SHG-44,筛选能够与CCND1协同抑制胶质母细胞瘤细胞增殖的化学治疗药物。方法用蛋白质印迹法检测CCND1表达沉默及过表达的人源性胶质母细胞瘤细胞株SHG-44中多药耐药基因MDR1的表达产物P-糖蛋白(P-gp)及凋亡因子Bcl-2、Caspase-3的表达。使用卡莫司汀(BCNU)、洛莫司汀(CCNU)、替莫唑胺(TMZ)3种化学治疗药物分别处理CCND1过表达或表达沉默的SHG-44细胞,筛选能够与CCND1表达沉默协同抑制肿瘤细胞生长的化学治疗药物,并在人源性胶质母细胞瘤细胞株系U251中进一步验证。结果蛋白质印迹结果示CCND1表达沉默能够下调P-gp、Bcl-2的表达,上调Caspase-3的表达(P均<0.01)。BCNU(0.05、0.25μg/mL)、CCNU(20、80μg/mL)处理CCND1过表达或表达沉默的SHG-44细胞的第2、3、4、5天时,细胞生长曲线的差异均无统计学意义;而在药物处理后细胞培养的第4、5天,CCND1表达沉默SHG-44细胞的生长受到TMZ(9.1μg/mL)的抑制作用较亲代SHG-44细胞强(P<0.05)。U251细胞实验证实CCND1表达沉默促进TMZ的化学治疗敏感性。结论 CCND1表达沉默联合TMZ较两者单独作用能更有效地抑制人源性胶质母细胞瘤细胞株SHG-44的增殖,提示CCND1可能参与TMZ化学治疗耐药机制。
ObjectiveTo screen chemotherapeutic drugs that can synergistically inhibit the proliferation of glioblastoma cells with CCND1by constructing CCND1silenced and overexpressed human glioblastoma cell lines SHG44.MethodsSHG44cells with CCND1silenced or overexpressed were constructed,and the expression of P glycoprotein(P gp,expression product of multidrug resistance gene MDR1)and apoptotic factors(Bcl2,Caspase3)in the cells were detected by Western blotting.The SHG44cells with CCND1silenced or overexpressed were cultured with carmustine(BCNU),lomustine(CCNU)and temozolomide(TMZ),respectively;and then the available chemotherapeutic drugs were screened,which could synergistically inhibit the proliferation of tumor cells with CCND1sliencing.Human glioblastoma cell lines U251were used to verify the findings in SHG44cells.ResultsWestern blotting analysis showed that CCND1silencing significantly down regulated the expressions of MDR1and Bcl2,and up regulated the expression of Caspase3(all P<0.01).There were no significant differences in cell growth curves between the CCND1silenced cells treating with BCNU(0.05μg/mL,0.25μg/mL)and CCNU(20μg/mL,80μg/mL)for2,3,4,and5days;However,the proliferation of CCND1silenced SHG44cells was significantly inhibited by TMZ(9.1μg/mL)compared with parent SHG44cells on the4th and5th day after treatment(P<0.05).The findings that CCND1silencing promoted chemosensitivity of TMZ were confirmed by U251cell experiments.ConclusionCCND1silencing combined with TMZ is more effective in inhibiting the proliferation of human glioblastoma cell lines SHG44than CCND1silencing or TMZ alone,suggesting that CCND1may be involved in chemotherapeutic resistance of glioblastoma cells to TMZ.
作者
赵玮
张丹枫
王君玉
董艳
吴小军
胡国汉
骆纯
卢亦成
ZHAO Wei;ZHANG Dan-feng;WANG Jun-yu;DONG Yan;WU Xiao-jun;HU Guo-han;LUO Chun;LU Yi-cheng(Department of Neurosurgery,Changzheng Hospital,Second Military Medical University,Institute of Shanghai Neurosurgical Research, Shanghai 200003,China;Department of General Surgery,General Hospital of Rocket Force of PLA,Beijing 100088,China)
出处
《第二军医大学学报》
CAS
CSCD
北大核心
2017年第12期1503-1507,共5页
Academic Journal of Second Military Medical University
