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首页> 外文期刊>Journal of experimental & clinical cancer research : >CCL3 and CCL20-recruited dendritic cells modified by melanoma antigen gene-1 induce anti-tumor immunity against gastric cancer ex vivo and in vivo
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CCL3 and CCL20-recruited dendritic cells modified by melanoma antigen gene-1 induce anti-tumor immunity against gastric cancer ex vivo and in vivo

机译:黑色素瘤抗原基因1修饰的CCL3和CCL20诱导的树突状细胞体外和体内诱导抗胃癌的抗肿瘤免疫力

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Background To investigate whether dendritic cell (DC) precursors, recruited by injection of chemokine ligand 3 (CCL3) and CCL20 , induce anti-tumor immunity against gastric cancer induced by a DC vaccine expressing melanoma antigen gene-1 (MAGE-1) ex vivo and in vivo. Methods B6 mice were injected with CCL3 and CCL20 via the tail vein. Freshly isolated F4/80-B220-CD11c+ cells cultured with cytokines were analyzed by phenotype analysis and mixed lymphocyte reaction (MLR). For adenoviral (Ad)-mediated gene transduction, cultured F4/80-B220-CD11c+ cells were incubated with Ad-MAGE-1. Vaccination of stimulated DC induced T lymphocytes. The killing effect of these T cells against gastric carcinoma cells was assayed by MTT. INF-γ production was determined with an INF-γ ELISA kit. In the solid tumor and metastases model, DC-based vaccines were used for immunization after challenge with MFC cells. Tumor size, survival of mice, and number of pulmonary metastatic foci were used to assess the therapeutic effect of DC vaccines . Results F4/80-B220-CD11c+ cell numbers increased after CCL3 and CCL20 injection. Freshly isolated F4/80-B220-CD11c+ cells cultured with cytokines were phenotyically identical to typical DC and gained the capacity to stimulate allogeneic T cells. These DCs were transduced with Ad-MAGE-1, which were prepared for DC vaccines expressing tumor antigen. T lymphocytes stimulated by DCs transduced with Ad-MAGE-1 exhibited specific killing effects on gastric carcinoma cells and produced high levels of INF-γ ex vivo. In vivo, tumor sizes of the experimental group were much smaller than both the positive control group and the negative control groups (P P Conclusions CCL3 and CCL20 -recruited DCs modified by adenovirus-trasnsduced, tumor-associated antigen, MAGE-1, can stimulate anti-tumor immunity specific to gastric cancer ex vivo and in vivo. This system may prove to be an efficient strategy for anti-tumor immunotherapy.
机译:背景为了研究是否通过注射趋化因子配体3(CCL3)和CCL20募集的树突状细胞(DC)前体是否诱导针对表达黑素瘤抗原基因1(MAGE-1)的DC疫苗诱导的胃癌抗肿瘤免疫力。和体内。方法B6小鼠经尾静脉注射CCL3和CCL20。通过表型分析和混合淋巴细胞反应(MLR)分析了新鲜分离的F4 / 80 - B220 - CD11c + 细胞。对于腺病毒(Ad)介导的基因转导,将培养的F4 / 80 - B220 - CD11c + 细胞与Ad-MAGE-1一起孵育。刺激的DC诱导T淋巴细胞的疫苗接种。通过MTT测定这些T细胞对胃癌细胞的杀伤作用。使用INF-γELISA试剂盒确定INF-γ的产生。在实体瘤和转移模型中,使用DC疫苗接种MFC细胞后进行免疫。肿瘤大小,小鼠存活率和肺转移灶数量用于评估DC疫苗的治疗效果。结果注射CCL3和CCL20后F4 / 80 - B220 - CD11c + 细胞数增加。用细胞因子培养的新鲜分离的F4 / 80 - B220 - CD11c + 细胞在表型上与典型DC相同,并具有刺激同种异体T细胞的能力。这些DC用Ad-MAGE-1转导,Ad-MAGE-1被制备用于表达肿瘤抗原的DC疫苗。用Ad-MAGE-1转导的DC刺激的T淋巴细胞对胃癌细胞具有特异性杀伤作用,并且离体产生高水平的INF-γ。在体内,实验组的肿瘤大小远小于阳性对照组和阴性对照组(PP结论:腺病毒转导的肿瘤相关抗原MAGE-1修饰的CCL3和CCL20诱导的DC可以刺激抗胃癌离体和体内特异的抗肿瘤免疫力,该系统可能被证明是抗肿瘤免疫治疗的有效策略。

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