转染MIP-1α和B7-1基因增强小鼠抗淋巴瘤效应的初步研究
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南京军区医学科学技术研究“十一五”计划课题(编号:07Z034);福建省自然科学基金(编号:2010J01221)资助。


Preliminary Study of MIP-1α and B7-1 gene Transfection Enhances Antitumor Effection on Mouse Lymphoma
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    摘要:

    【摘要】 目的 观察转染趋化因子MIP-1α和共刺激分子B7-1基因增强小鼠抗淋巴瘤的效应。方法 将MIP-1α和B7-1基因慢病毒重组载体转染小鼠EL-4淋巴瘤细胞,应用RT-PCR检测MIP-1α和B7-1基因mRNA表达,Western blot法检测MIP-1α和B7-1蛋白表达;转基因EL-4细胞注入小鼠右腋皮下,观察成瘤情况;灭活的转基因EL-4细胞注入成瘤小鼠体内,观察其增强小鼠抗淋巴瘤效应。结果RT-PCR检测发现EL-4/MIP-1α+B7-1细胞内有MIP-1α及B7-1mRNA表达,Western blot显示MIP-1α及B7-1蛋白表达;MIP-1α组、B7-1组较对照组成瘤时间延长,成瘤率降低,肿瘤平均体积较小,而联合组成瘤性消失;MIP-1α和B7-1治疗组的肿瘤平均体积、重量及肿瘤器官转移率明显小于对照组(P<0.05),而联合组的肿瘤平均体积及重量明显小于MIP-1α和B7-1组(P<0.05),而且联合组小鼠平均生存期,均较单基因组、对照组明显延长(P<0.05)。结论 转染MIP-1α和B7-1基因能够明显增强小鼠机体抗淋巴瘤效应,明显延长荷瘤小鼠的平均生存期,为淋巴瘤的基因治疗提供了新的思路。

    Abstract:

    【ABSTRACT】 Objective To research the antitumor effection.of MIP-1α and B7-1 gene transfection. on mouse lymphoma. Methods Lentivirus-mediated mouse MIP-1α and B7-1 gene vectors . infected EL-4 cells. The MIP-1α和B7-1 mRNA were identified by RT-PCR and. MIP-1α和B7-1 protein were examined by Western blot. Then the infected EL-4 cells were injected into right armpits of mouse, and observed the development of tumor. The transfected EL-4 cells were infected to tumor-bearing mice, and observe the antitumor effection. Results RT-PCR assay showed that there were MIP-1αand B7-1 mRNA in the EL-4/MIP-1α+B7-1 cells, as well as MIP-1αand B7-1 protein examined by Western blot. MIP-1α and B7-1 group occupied much more time than the control group in the tumor generation, and which mean tumor volume was also smaller than the control group, as well as the rate of tumor formation, however there were no tumor generation in unite group. The average tumor volume,weight and organ involvement rate of MIP-1 α and B7-1 group was significantly smaller than that of the control group ( P < 0.05 ), while the average tumor volume and weight of united group was also significantly smaller than that of MIP-1 α and B7-1 group ( P < 0.05 ). In addition, the mean survival time of unite group was significantly longer than single group, and the control group ( P < 0.05 ). .Conclusion Lentivirus-mediated mouse MIP-1α and B7-1 gene transfection could effectively enhance the anti-lymphoma effection in tumor-bearing mice, and significantly prolonged the average survival time. Which also provided a new idea for the lymphoma gene therapy .

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刘伟,余英豪.转染MIP-1α和B7-1基因增强小鼠抗淋巴瘤效应的初步研究[J].中国比较医学杂志,2013,23(6).

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  • 收稿日期:2013-04-01
  • 最后修改日期:2013-04-22
  • 录用日期:2013-04-23
  • 在线发布日期: 2013-07-02
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