Atienza C, Elliott M J, Dong Y B, Yang H L, Stilwell A, Liu T J, McMasters K M
Department of Surgery, Division of Surgical Oncology, University of Louisville School of Medicine, J. Graham Brown Cancer Center, Louisville, Kentucky 40202, USA.
Int J Mol Med. 2000 Jul;6(1):55-63. doi: 10.3892/ijmm.6.1.55.
E2F -1 is a transcription factor that regulates cell cycle progression into S-phase. Deregulation of E2F-1 activity has been associated with cellular commitment to apoptosis. Also critical in the regulation of S-phase are the actions of the cyclin dependent kinases, Cdk2 and cdc2. Inhibition of these cyclin dependent kinases has been similarly associated with disrupting orderly S-phase progression and causing subsequent apoptosis in certain cancer cells. In this study, we examine the ability of adenovirus-mediated E2F-1 overexpression to induce apoptosis in human gastric carcinoma cells. Furthermore, we investigate the effect of the cyclin dependent kinase inhibitors, olomoucine and roscovitine, on E2F-1-mediated apoptosis in human gastric carcinoma cells. AGS and SNU-1 gastric adenocarcinoma cells were infected with adenoviral vectors expressing E2F-1 (Ad5CMVE2F-1) or control viruses expressing beta-galactosidase (Ad5CMVLacZ) or lacking a transgene (Ad5). Gastric adenocarcinoma cells were then independently treated with roscovitine or olomoucine. Finally, gastric adenocarcinoma cells were infected with the various adenoviral vectors in combination with roscovitine or olomoucine. E2F-1 overexpression resulted in an 85% reduction in cell viability at 72 h compared to controls. Combining E2F-1 overexpression with roscovitine resulted in >99% reduction in cell viability by 72 h. Overexpression of E2F-1 resulted in premature S-phase entry and G2/M arrest at 24 h, followed by apoptosis by 72 h. Combining E2F-1 overexpression with roscovitine resulted in an earlier G2/M arrest, followed by a more complete, widespread apoptotic response by 24 h. Caspase 3/CPP32 activation and PARP cleavage in response to E2F-1 overexpression, alone and in combination with roscovitine, implicate the caspase cascade in E2F-1-mediated apoptosis of gastric cancer cells. Bax levels also increased in response to E2F-1 gene transfer, alone and in combination with roscovitine. E2F-1 overexpression induces widespread apoptosis in human gastric carcinoma cells. Combining E2F-1 overexpression with cyclin-dependent kinase inhibitors results in an enhanced apoptotic response, causing nearly complete gastric tumor cell death within 72 h. E2F-1 gene therapy in combination with cyclin dependent kinase inhibitors is a potentially active chemogene therapy strategy for the treatment of human gastric cancer.
E2F -1是一种调节细胞周期进入S期的转录因子。E2F-1活性失调与细胞凋亡相关。细胞周期蛋白依赖性激酶Cdk2和cdc2在S期调节中也起关键作用。抑制这些细胞周期蛋白依赖性激酶同样与破坏S期的有序进程以及在某些癌细胞中导致随后的凋亡有关。在本研究中,我们检测腺病毒介导的E2F-1过表达诱导人胃癌细胞凋亡的能力。此外,我们研究细胞周期蛋白依赖性激酶抑制剂olomoucine和roscovitine对人胃癌细胞中E2F-1介导的凋亡的影响。AGS和SNU-1胃腺癌细胞用表达E2F-1的腺病毒载体(Ad5CMVE2F-1)或表达β-半乳糖苷酶的对照病毒(Ad5CMVLacZ)或缺乏转基因的病毒(Ad5)感染。然后胃腺癌细胞分别用roscovitine或olomoucine处理。最后,胃腺癌细胞用各种腺病毒载体与roscovitine或olomoucine联合感染。与对照相比,E2F-1过表达导致72小时时细胞活力降低85%。E2F-1过表达与roscovitine联合使用导致72小时时细胞活力降低>99%。E2F-1过表达导致24小时时过早进入S期并停滞在G2/M期,随后72小时时发生凋亡。E2F-1过表达与roscovitine联合使用导致更早的G2/M期停滞,随后24小时时出现更完全、广泛的凋亡反应。单独及与roscovitine联合使用时,E2F-1过表达引起的半胱天冬酶3/CPP32激活和PARP裂解表明半胱天冬酶级联反应参与E2F-1介导的胃癌细胞凋亡。单独及与roscovitine联合使用时,Bax水平也因E2F-1基因转导而升高。E2F-1过表达诱导人胃癌细胞广泛凋亡。E2F-1过表达与细胞周期蛋白依赖性激酶抑制剂联合使用导致凋亡反应增强,在72小时内导致几乎完全的胃肿瘤细胞死亡。E2F-1基因治疗与细胞周期蛋白依赖性激酶抑制剂联合使用是一种治疗人胃癌的潜在有效的化学基因治疗策略。
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