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机构地区:[1]中山医科大学肿瘤防治中心,广东广州510060
出 处:《癌症》2001年第4期363-367,共5页Chinese Journal of Cancer
基 金:国家自然科学基金项目!( NO.39770840)
摘 要:目的:探讨以拓扑异构酶 I抑制剂羟基喜树碱( 10- hydroxycampothecin,HCPT)为基础的联合方案对实验性鼻咽癌 (nasopharyngeal carcinoma,NPC)的抗瘤作用。方法:以人 NPC细胞株 CNE2的体外和裸鼠移植瘤为模型,研究 HCPT与顺铂( cisplatin,DDP)或(和) 5-氟尿嘧啶( 5- fluorouracil,5- FU)联合作用的抗瘤效果。细胞毒测定用 MTT法,体内抗瘤模型为 CNE2裸鼠移植瘤模型。结果: HCPT、 DDP和 5- FU对 CNE2的 IC50分别为 14.2、 17.2及 49.2μ mol/L。 HCPT与 DDP合用具有明显的协同抗 NPC作用。 HCPT与 5- FU合用虽较单药抗瘤作用优,但未见明显的相加或协同作用。 HCPT+ DDP+ 5- FU三药合用较两药合用效果更优,且毒性可以耐受。结论: HCPT+ DDP或 HCPT+ DDP+ 5- FU具有协同抗 NPC肿瘤作用,可试用于临床。Objective: This study was designed to evaluate topoisomerase I inhibitor 10- hydroxycampothecin- based combination chemotherapy for nasopharyngeal carcinoma (NPC) in vitro and in vivo. Methods: Antitumor activity of 10- hydroxycampothecin (HCPT) in combination with 5- fluorouracil (5- FU) and/or cisplatin (DDP) in NPC cell line CNE2 and in CNE2 xenograft of nude mice were determined. The cytotoxicity was measured by MTT assay. Results: HCPT, 5- FU,and DDP had potential cytotoxicity to CNE2 cells. Their IC50 were 14.2μ mol/L, 17.2μ mol/L, 49.2μ mol/L,respectively. HCPT in combination with DDP had significant anticancer effect for NPC in vitro and in vivo. But no significant additivity or synergism was showed in the combination of HCPT with 5- FU in vitro and in vivo. HCPT+ DDP+ 5FU was much better than HCPT+ DDP for chemotherapy of NPC and the toxicity was endurable in the nude mice bearing CNE2 xenograft. Conclusion: HCPT+ DDP and HCPT+ DDP+ 5- FU were potential regimen for chemotherapy of NPC.
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