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首页> 外文期刊>The journal of gene medicine >Advantages and limitations of particle-mediated transfection (gene gun) in cancer immuno-gene therapy using IL-10, IL-12 or B7-1 in murine tumor models
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Advantages and limitations of particle-mediated transfection (gene gun) in cancer immuno-gene therapy using IL-10, IL-12 or B7-1 in murine tumor models

机译:在小鼠肿瘤模型中使用IL-10,IL-12或B7-1进行癌症免疫基因治疗时,粒子介导的转染(基因枪)的优缺点

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Background Previous studies have shown that particle-mediated transfection (PMT; gene gun) is an efficient method of non-viral gene transfer. We have examined the advantages and limitations of PMT in cancer immuno-gene therapy using IL-10, IL-12 or B7-1, all of which have been shown to be effective in murine tumor models using retroviral vectors. Methods Murine cell lines (MCA205, MCA207, NIH-3T3) were treated with in vitro PMT, liposome-mediated transfection (LMT) or retroviral transfection. In vivo PMT was also examined for in vivo experiments using C57BL/6. ResultsTransfection efficiency and cytokine expression of PMT were similar to those of LMT, another non-viral approach, in culture when murine adherent cells were used. Tumor establishment of MCA205 was suppressed when they were transfected with the mIL-12 and/or mB7-1 gene using PMT in vitro. In a treatment of established tumor, vaccination with tumor cells transfected with an IL-12 gene suppressed tumor growth, whereas a B7-1 gene was not effective. When an IL-10 gene was used to supply a high level of expression for antitumor effects, neither in vitro nor in vivo PMT could suppress even tumor establishment. These failures appear to be caused by the characteristics of PMT which allows high, but transient, expression of transfected genes. ConclusionsParticle-mediated transfection is a useful non-viral transfection method in a system which does not require high-level gene expression for a prolonged time of period.
机译:背景技术以前的研究表明,粒子介导的转染(PMT;基因枪)是一种非病毒基因转移的有效方法。我们已经检查了PMT在使用IL-10,IL-12或B7-1的癌症免疫基因治疗中的优势和局限性,所有这些都已被证明在使用逆转录病毒载体的鼠类肿瘤模型中有效。方法采用体外PMT,脂质体介导的转染(LMT)或逆转录病毒转染处理小鼠细胞系(MCA205,MCA207,NIH-3T3)。还使用C57BL / 6检查了体内PMT的体内实验。结果在使用鼠类贴壁细胞的培养中,PMT的转染效率和细胞因子表达与另一种非病毒方法LMT相似。当在体外使用PMT将mIL-12和/或mB7-1基因转染时,MCA205的肿瘤形成受到抑制。在已建立的肿瘤的治疗中,用IL-12基因转染的肿瘤细胞进行的疫苗接种抑制了肿瘤的生长,而B7-1基因无效。当使用IL-10基因提供高水平的抗肿瘤作用时,无论是体外还是体内的PMT都不能抑制甚至肿瘤的形成。这些失败似乎是由于PMT的特性引起的,该特性允许高但瞬时表达转染的基因。结论颗粒介导的转染是一种不需要长时间的高水平基因表达的系统中有用的非病毒转染方法。

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