临床肿瘤学杂志

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AFP介导慢病毒载体治疗荷人肝癌裸鼠移植瘤的实验研究

王轩,王欣,袁振华,夏冰祥,张业伟   

  1. 210009 南京 南京医科大学附属肿瘤医院普外科
  • 收稿日期:2015-07-14 修回日期:2015-09-08 出版日期:2015-11-30 发布日期:2015-11-30

The experimental study of AFP-mediated lentivirus in human hepatocellular carcinoma bearing nude mice

WANG Xuan,WANG Xin,YUNA Zhenhua,XIA Bingxiang,ZHANG Yewei   

  1. Department of General Surgery,Affiliated Tumor Hospital of Nanjing Medical University, Nanjing 210009,China
  • Received:2015-07-14 Revised:2015-09-08 Online:2015-11-30 Published:2015-11-30

摘要: 目的 构建甲胎蛋白(AFP)介导的以沉默胰岛素样生长因子1型受体(IGF1R)和表达野生型p53(Wtp53)的重组慢病毒,探讨该慢病毒载体对肝癌干细胞CD45-CD90+双靶点基因系统(IGF1R和Wtp53)和对体内肝癌生长的抑制作用。方法 从肝癌细胞Hep3B系中分离出肝癌干细胞CD45-CD90+细胞亚群,用携带AFP-Wtp53-pPRIME-miR30-shRNA-IGF1R融合基因的慢病毒进行体外转染。利用RT-PCR和Western blotting检测IGF1R、WtP53在细胞内的表达,将荷人肝癌的移植瘤裸鼠随机分为空白对照组(腋下接种未感染任何病毒的CD45-CD90+细胞)、空载体对照组(腋下接种感染空载体慢病毒pPRIME的CD45-CD90+细胞)和实验组(腋下接种感染空载体慢病毒AFP-WtP53-pPRIME-miR30-shRNA-IGF1R的CD45-CD90+细胞),检测各组的IGF1R表达,微血管密度和细胞凋亡程度。结果 成功构建anti-AFP介导的慢病毒;qRT-PCR和Western blotting检测显示,anti-AFP介导的慢病毒能表达Wtp53并同时干扰IGF1R的表达。体内实验显示,与空白对照组和空载体对照组相比,实验组肿瘤的潜伏期较长,肿瘤体积较小,瘤组织的IGF1R水平、微血管密度较低,但凋亡指数较高,差异有统计学意义(P<0.05)。结论 anti-AFP介导的慢病毒可高效特异性转染肝癌干细胞CD45-CD90+ 双靶点基因系统,起到杀伤肝癌干细胞及抑制肝癌体内生长的作用。

Abstract: Objective To construct the alpha-fetroprotein(AFP) mediated lentivirus in order to silence the expression of insulin like growth factor 1 receptor (IGF1R) and over-express p53 (Wtp53), and to explore the effect of lentivirus on the double target gene system (IGF1R and Wtp53)of liver cancer stem cells CD45-CD90+ and growth of liver cancer in vivo. Methods Liver cancer stem cells CD45-CD90+ were isolated from Hep3B cells. The lentivirus carrying the fusion genes of AFP-Wtp53-pPRIME-miR30-shRNA-IGF1R were used for in vitro transfection. Western blotting and RT-PCR were used to detect the expressions of wtp53 and IGF1R in the cells. The transplanted tumor model was established in BALB-C nude mice and then randomly divided into the blank control group (axillary inoculation with CD45-CD90+ cells), empty vector control group (axillary inoculation with CD45-CD90+ cells infected with empty vector pPRIME)and experimental group(axillary inoculation with CD45-CD90+ cells infected with AFP-Wtp53-pPRIME-miR30-shRNA-IGF1R). The IGF1R expression, microvessel density and apoptosis in each group were detected. Results The anti-AFP mediated lentivirus was successfully constructed. The Results of qRT-PCR and Western blotting showed that the recombinant lentivirus can over-express Wtp53 and interfere the expression of IGF1R. In vivo experiments showed that in comparison with the blank control group and empty vector control group, there were longer incubation period, smaller tumor volume, lower level of IGF1R and microvessel density in tumor tissue and higher apoptosis index in experimental group(P<0.05). Conclusion Anti-AFP mediated lentivirus targeted double target gene system of CD45-CD90+ cells presents high efficiency and specificity, playing a role in the growth of liver cancer stem cells and inhibits the growth of liver cancer cells.

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