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作 者:肖小平[1] 李月琴[1] 徐彬[1] 李弘剑[1] 张欣[1] 周天鸿[1] 邹奕[1]
机构地区:[1]暨南大学生命科学技术学院生物化学与分子生物学实验室,广东广州510632
出 处:《中国病理生理杂志》2009年第7期1254-1261,共8页Chinese Journal of Pathophysiology
基 金:国家自然科学基金资助项目(No.90608024);广东省自然科学基金资助项目(No.81510632;No.010000013);教育部科学技术研究重点资助项目(No.207144)
摘 要:目的:研究转基因SSTR2对有不同内源性SSTRs表达谱的癌细胞增殖抑制及其潜在信号途径。方法:在裸鼠身上接种过表达SSTR2或LacZ的capan-2cell和A549细胞,观察肿瘤生长情况。在裸鼠身上构建capan-2移植瘤模型,通过皮下注射携带SSTR2基因的腺病毒,观察肿瘤生长情况。免疫印迹法分析可能涉及的信号途径。结果:过表达SSTR2能够抑制具有不同内源性SSTRs表达谱肿瘤的生长,包括capan-2具有内源性SSTR2表达。SSTR2过表达明显影响了凋亡途径、MAPK途径以及血管生成中的一些组件。结论:SSTR2有希望成为使用转基因治疗多数癌症的候选基因。AIM: To study the anti - proliferation effect of overexpressed SSTR2 in experimental cancer with different profiles of endogenous SSTRs expressions and the possible signaling pathways involved. METHODS: In the first experiment, the growth of the tumor xenografts of the inoculated capan - 2 cells and A549 cells overexpressing SSTR2 or LacZ was investigated in nude mice. In the second experiment, the adenoviral vector expressing SSTR2 were introduced into experimental capan -2 xenografts by intratumoral injection. The growth inhibition of these experiment tumors was observed and the potential influences on different signaling pathways were analyzed by immunoassays. RESULTS: Overexpression of SSTR2 inhibited the growth of tumors with different profiles of endogenous SSTRs, including experimental capan - 2 xenografts that had endogenous SSTR2 expression. Overexpression significantly affected a number of components in apoptotic pathway, MAPK pathway and angiogenesis. CONCLUSION: SSTR2 is a promising candidate for gene therapy in a wide spectrum of cancers.
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