| 低氧提高肿瘤细胞反义VEGF165基因表达 |
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| 引用本文: | 郭文忠 冉宇靓 等. 低氧提高肿瘤细胞反义VEGF165基因表达[J]. Acta biochimica et biophysica Sinica, 2002, 34(5): 625-629 |
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| 作者姓名: | 郭文忠 冉宇靓 等 |
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| 作者单位: | 中国医学科学院肿瘤研究所细胞生物学及分子生物学室,中国协和医科大学肿瘤研究所细胞生物学及分子生物学室 北京100021,北京100021 |
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| 摘 要: | 为了探讨反义VEGF1 65基因对食管癌的抑制作用 ,并初步探讨利用肿瘤低氧微环境改善基因治疗的效果 ,采用PCR技术和DNA重组技术构建了含低氧反应元件的真核表达载体 ,并用此载体构建了含荧光素酶报告基因和反义VEGF1 65基因的重组载体。用脂质体将重组载体导入食管癌细胞 ,体外用化学发光光度计测定低氧对报告基因表达的调节和ELISA法间接测定低氧对反义VEGF基因表达的调节作用。体内利用裸鼠皮下移植实验研究低氧对反义VEGF1 65基因抑瘤作用的影响。体外实验表明 ,用带低氧反应元件的重组真核表达载体转染食管癌细胞 ,在低氧培养下可以使报告基因的表达提高 3 780 % ,并可以显著提高反义VEGF1 65基因的表达 ,体内用带低氧反应元件的载体将反义VEGF1 65基因导入食管癌细胞中 ,其抑瘤效果显著优于不含该元件的载体 ,抑瘤率分别为 71 .7%和 5 6 .1 %。反义VEGF1 65基因能显著抑制食管癌的生长 ;利用肿瘤低氧可以实现治疗基因的自主调节 ,改善基因治疗的效果
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| 关 键 词: | 食管癌 血管形成 低氧 血管内皮生长因子 |
Enhancement by Hypoxia of Antisense VEGF_(165) Gene Expression in Esophageal Cancer Cells |
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| GUO Wen Zhong,RAN Yu Liang,LIU Jun,YU Long,SUN Li Xin,YANG Zhi Hua. Enhancement by Hypoxia of Antisense VEGF_(165) Gene Expression in Esophageal Cancer Cells[J]. Acta biochimica et biophysica Sinica, 2002, 34(5): 625-629 |
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| Authors: | GUO Wen Zhong RAN Yu Liang LIU Jun YU Long SUN Li Xin YANG Zhi Hua |
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| Affiliation: | GUO Wen Zhong,RAN Yu Liang,LIU Jun,YU Long,SUN Li Xin,YANG Zhi Hua * |
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| Abstract: | To demonstrate effects of antisense VEGF 165 to suppress esophageal cancer cells and to improve efficacy of the gene therapy of tumor by using hypoxic environment, hypoxia response element(HRE) was cloned from promoter of VEGF by PCR and employed to construct an eukaryotic expression vector containing luciferase and antisense VEGF 165 by using recombinant DNA techniques. The recombinant vectors were transfered into esophageal cancer cells by lipofectin methods, and hypoxia inducible reporter gene expression was determined by luminometer and the expression of antisense VEGF was evaluated indirectly by ELISA that detected of VEGF. The esophageal cells tansfected by antisense VEGF 165 gene were transplanted into nude mice, in order to evaluate the suppressive effect of antisense VEGF 165 . Our results showed that, in vitro , hypoxia increased expression of reporter gene to 3 780% and enhanced greatly expression of antisense VEGF. In vivo , the growth of esophageal cancer cells transfected by antisense VEGF in the vector containing HRE was suppressed more significantly, with suppression rate being 71.1%, than that by the vector without HRE, whose inhibiting rate 56.1%. It was concluded that antisense VEGF 165 suppressed significantly growth of esophageal cancer, and by using a gene expression vector containing HRE, the expression of target genes could be regulated autonomously by hypoxic environment of tumor and the efficiency of gene therapy could be greatly improved. |
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| Keywords: | esophageal cancer angiogenesis hypoxia VEGF |
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