外源性野生型p53增强了单纯疱疹病毒胸苷激酶/丙氧鸟苷对C6胶质瘤细胞的抗肿瘤作用。
Exogenous wt-p53 enhances the antitumor effect of HSV-TK/GCV on C6 glioma cells.
作者信息
Huang Qiang, Pu Peiyu, Xia Zhibo, You Yongping
机构信息
Department of Neurosurgery, Tianjin Medical University General Hospital, 154 Anshan Road, Tianjin, 300052, People's Republic of China.
出版信息
J Neurooncol. 2007 May;82(3):239-48. doi: 10.1007/s11060-006-9279-x. Epub 2006 Nov 11.
OBJECTIVE
To study on the antitumor effect of combining wt-p53 gene with suicide gene therapy (HSV-tk+GCV) for malignant gliomas.
METHODS
AdCMV-p53 was transfected into C6 glioma cells at MOI of (Multiplicity of infection) 0(G100), 10(TPG1), 100(TPG2), then AdCMV-tk was transducted to C6 glioma cells of G100, TPG1 and TPG2, respectively, at MOI of 100. The C6 glioma cells tranfected with both AdCMV-p53 and AdCMV-tk were exposed to various concentration of GCV. The cell survival rate was measured by MTT assay in vitro. Rat glioma model was established by injecting 5 x 10(5) C6 glioma cells into right caudate nucleus of SD rats. AdCMV-p53 and AdCMV-tk were injected into glioma on day 5 and 6, respectively. On day 7, ganciclovir (GCV) was administrated intraperitoneally at 15 mg/kg/day for 14 days. The survival time of all rats was observed. The growth of intracerebral tumors was monitored dynamically by enhanced MRI. Cell apoptosis was evaluated by TUNEL method. Expression of HSV-tk gene was identified by in situ hybridization and expression of exogenous p53 gene was detected with Western blotting.
RESULTS
In vitro, wt-p53 significantly enhanced antitumor effect of HSV-tk/GCV. The concentration of GCV for ID50 of TPG2 cells (0.001 microg/ml GCV) was 10 times lower than that for the cells of tk-GCV group (MOI = 100), while the concentration of GCV for ID100 of TPG2 (0.01 microg/ml GCV) and TPG1(0.1 microg/ml GCV) was 100 and 10 times lower than that for the cells of tk-GCV group (MOI = 100), respectively. Apoptosis of C6 glioma cells also could be induced by transfection with wt-p53 gene slightly. For in vivo study, the survival time of tumor-bearing rats treated with HSV-TK/GCV or wt-p53 combined with HSV-TK/GCV was significantly prolonged and the intracerebral tumors were regressed and disappeared earlier in the combined gene therapy group than those in the HSV-TK/GCV therapy group as shown in enhanced MRI. However, only half dose of GCV for the rats treated with both wt-p53 and HSV-TK/GCV was needed to obtain the same efficacy as those rats treated with HSV-TK/GCV alone. These results indicate that the transfection of wt-p53 potentiates the effect of HSV-TK/GCV therapy.
CONCLUSIONS
The combination of HSV-tk/GCV system with wt-p53 gene transduction is optimal for clinical therapeutic trials of suicide gene therapy for malignant gliomas.
目的
研究野生型p53基因与自杀基因疗法(单纯疱疹病毒胸苷激酶基因+更昔洛韦,HSV-tk+GCV)联合应用对恶性胶质瘤的抗肿瘤作用。
方法
以感染复数(MOI)为0(G100)、10(TPG1)、100(TPG2)将腺病毒介导的人野生型p53基因(AdCMV-p53)转染至C6胶质瘤细胞,然后分别以MOI为100将腺病毒介导的单纯疱疹病毒胸苷激酶基因(AdCMV-tk)转导至G100、TPG1和TPG2的C6胶质瘤细胞。将同时转染AdCMV-p53和AdCMV-tk的C6胶质瘤细胞暴露于不同浓度的更昔洛韦(GCV)。采用MTT法体外检测细胞存活率。将5×10⁵个C6胶质瘤细胞注入SD大鼠右侧尾状核建立大鼠胶质瘤模型。分别于第5天和第6天向胶质瘤内注射AdCMV-p53和AdCMV-tk。第7天,腹腔注射更昔洛韦(GCV),剂量为15mg/kg/天,共14天。观察所有大鼠的生存时间。通过增强磁共振成像(MRI)动态监测脑内肿瘤生长。采用末端脱氧核苷酸转移酶介导的缺口末端标记法(TUNEL法)评估细胞凋亡。通过原位杂交鉴定HSV-tk基因表达,采用蛋白质免疫印迹法检测外源性p53基因表达。
结果
体外实验中,野生型p53显著增强了HSV-tk/GCV的抗肿瘤作用。TPG2细胞半数抑制浓度(ID50)所需的GCV浓度(0.001μg/ml GCV)比单纯tk-GCV组(MOI = 100)细胞低10倍,而TPG2(0.01μg/ml GCV)和TPG1(0.1μg/ml GCV)细胞完全抑制浓度(ID100)所需的GCV浓度分别比单纯tk-GCV组(MOI = 100)细胞低100倍和10倍。转染野生型p53基因也能轻微诱导C6胶质瘤细胞凋亡。体内实验研究中,如增强MRI所示,单纯HSV-TK/GCV治疗组或野生型p53联合HSV-TK/GCV治疗组荷瘤大鼠的生存时间显著延长,联合基因治疗组脑内肿瘤消退和消失时间比HSV-TK/GCV治疗组更早。然而,野生型p53和HSV-TK/GCV联合治疗的大鼠仅需一半剂量的GCV就能获得与单纯HSV-TK/GCV治疗大鼠相同的疗效。这些结果表明,野生型p53基因转染增强了HSV-TK/GCV疗法的效果。
结论
HSV-tk/GCV系统与野生型p53基因转导联合应用是恶性胶质瘤自杀基因疗法临床治疗试验的最佳选择。
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