首页> 外文期刊>The journal of immunology >Superior Protective and Therapeutic Effects of IL-12 and IL-18 Gene-Transduced Dendritic Neuroblastoma Fusion Cells on Liver Metastasis of Murine Neuroblastoma
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Superior Protective and Therapeutic Effects of IL-12 and IL-18 Gene-Transduced Dendritic Neuroblastoma Fusion Cells on Liver Metastasis of Murine Neuroblastoma

机译:IL-12和IL-18基因转导的树突状神经母细胞瘤融合细胞对小鼠神经母细胞瘤肝转移的优异保护作用

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Fusion vaccine of dendritic cells (DCs) and tumor cells has the advantage of inducing an immune response against multiple tumor Ags, including unknown tumor Ags. Using the liver metastasis model of C1300 neuroblastoma cells, we assessed the protective and therapeutic effects of fusion cells transduced with the IL-12 gene and/or the IL-18 gene. Improving the fusion method by combining polyethylene glycol and electroporation increased loading efficiency. In the A/J mice vaccinated with fusion cells modified with the LacZ gene (fusion/LacZ), IFN-γ production and CTL activity increased significantly compared with that of DCs/LacZ, C1300/LacZ, or a mixture of the two (mixture/LacZ). With the transduction of IL-12 and IL-18 genes into the fusion cells (fusion/IL-12/IL-18), the level of IFN-γ increased more than five times that of other fusion groups. In addition, NK cell activity and CTL activity increased significantly compared with that of mixture/LacZ, fusion/LacZ, DC/LacZ, or C1300/LacZ. In the protective and therapeutic studies of fusion cell vaccine, mice vaccinated with fusion/LacZ, fusion/IL-12, fusion/IL-18, or fusion/IL-12/IL-18 showed a significant decrease in liver metastasis and a significant increase in survival compared with mice given a mixture/LacZ, DCs/LacZ, or C1300/LacZ. In particular, the mice receiving fusion/IL-12/IL-18 vaccine showed a complete protective effect and the highest therapeutic effects. The present study investigates the improved loading efficiency of fusion cells and suggests that the introduction of IL-12 and IL-18 genes can induce extremely strong protective and therapeutic effects on liver metastasis of neuroblastoma.
机译:树突状细胞(DCs)和肿瘤细胞的融合疫苗具有诱导针对多种肿瘤Ag(包括未知肿瘤Ag)的免疫反应的优势。使用C1300神经母细胞瘤细胞的肝转移模型,我们评估了用IL-12和/或IL-18基因转导的融合细胞的保护和治疗作用。通过将聚乙二醇和电穿孔相结合来改善融合方法,可提高装载效率。与DCs / LacZ,C1300 / LacZ或两者的混合物(混合物)相比,接种了LacZ基因修饰的融合细胞(fusion / LacZ)的A / J小鼠的IFN-γ产生和CTL活性显着增加/ LacZ)。通过将IL-12和IL-18基因转导至融合细胞(fusion / IL-12 / IL-18),IFN-γ的水平增加了超过其他融合组的五倍。此外,与混合物/ LacZ,融合/ LacZ,DC / LacZ或C1300 / LacZ相比,NK细胞活性和CTL活性显着增加。在融合细胞疫苗的保护性和治疗性研究中,接种融合/ LacZ,融合/ IL-12,融合/ IL-18或融合/ IL-12 / IL-18的小鼠表现出肝转移的显着降低和与使用混合物/ LacZ,DCs / LacZ或C1300 / LacZ的小鼠相比,存活率提高了。特别地,接受融合/ IL-12 / IL-18疫苗的小鼠表现出完全的保护作用和最高的治疗作用。本研究调查了融合细胞的提高的装载效率,并建议引入IL-12和IL-18基因可以诱导对神经母细胞瘤肝转移的极强保护和治疗作用。

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