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首页> 外文期刊>The journal of gene medicine >Factors influencing immune response after in vivo retrovirus-mediated gene transfer to the liver
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Factors influencing immune response after in vivo retrovirus-mediated gene transfer to the liver

机译:体内逆转录病毒介导的基因转移到肝脏后影响免疫应答的因素

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Background Highly efficient retrovirus-mediated gene transfer into hepatocytes in vivo triggers an immune response directed against transduced hepatocytes. This effect may be due either to spreading of retroviral vectors in the blood stream with subsequent infection of antigen presenting cells (APCs) or to cross-presentation of the transgene product present as a contaminant in the viral stock. In order to decrease immune response, we evaluated the effect of asanguineous perfusion of the liver as well as purification of the viral stock on long-term transduction of hepatocytes using the nls-lacZ marker gene. Methods Animals were divided in four groups. In group 1, the viral supernatant was perfused in the regenerating liver after complete vascular exclusion of the organ. In group 2, using the same strategy, animals received retroviral supernatant that was passed through a β-galactosidase affinity column to reduce β-galactosidase contamination. In two control groups (respectively groups 3 and 4) the corresponding viral supernatants were delivered via peripheral injection. Results In group 1, 23.1% of animals had no immune response 2 months after gene delivery vs. 33.4% in group 2, 4.3% in control group 3, and 0% in control group 4. Statistical analysis of the results demonstrated that only the difference between groups 2 and 3 was statistically significant. This indicated that both asanguineous perfusion together with passage through an affinity column were required to decrease significantly immune response. Conclusions Our present results suggest that both supernatant contamination and viral spreading contribute to immune response after retrovirus-mediated gene delivery to the liver.
机译:背景技术在体内高效逆转录病毒介导的基因转移到肝细胞中会触发针对转导的肝细胞的免疫反应。这种作用可能是由于逆转录病毒载体在血流中扩散,随后又感染了抗原呈递细胞(APC),或者是由于在病毒原种中以污染物形式存在的转基因产物交叉呈递。为了降低免疫反应,我们使用nls-lacZ标记基因评估了肝脏的肝细胞灌注以及肝细胞的长期转导对病毒库的纯化作用。方法将动物分为四组。在第1组中,在器官完全被血管排斥后,在再生肝脏中灌注病毒上清液。在第2组中,使用相同的策略,动物接受逆转录病毒上清液,该上清液通过β-半乳糖苷酶亲和柱以减少β-半乳糖苷酶的污染。在两个对照组(分别是第3和第4组)中,通过外周注射递送相应的病毒上清液。结果在第1组中,基因递送后2个月无免疫反应的动物为23.1%,而第2组为33.4%,对照组3为4.3%,对照组4为0%。对结果的统计分析表明,只有第2组和第3组之间的差异具有统计学意义。这表明既需要大剂量灌注,又需要通过亲和柱,以显着降低免疫反应。结论我们目前的结果表明,在逆转录病毒介导的基因传递到肝脏后,上清液污染和病毒传播都有助于免疫反应。

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