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首页> 外文期刊>Cancer gene therapy >Concurrent delivery of tumor antigens and activation signals to dendritic cells by irradiated CD40 ligand-transfected tumor cells resulted in efficient activation of specific CD8|[plus]| T cells
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Concurrent delivery of tumor antigens and activation signals to dendritic cells by irradiated CD40 ligand-transfected tumor cells resulted in efficient activation of specific CD8|[plus]| T cells

机译:经辐射的CD40配体转染的肿瘤细胞向树突状细胞同时递送肿瘤抗原和激活信号导致特异性CD8 | + |的有效激活。 T细胞

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To improve the efficacy of tumor cell-based and dendritic cell (DC)-based cancer vaccines, this study explored the potential of a new cancer vaccine strategy, that is, the use of CD40 ligand-transfected tumor (CD40L-tumor) cells to simultaneously deliver both tumor-derived antigens (Ag) and maturation stimuli to DCs. Materials from frozen/thawed or irradiated human tumor cells, with or without surface CD40L, were internalized efficiently by immature DCs after coincubation. However, during the internalization process, only coculturing with irradiated CD40L-tumor cells resulted in concurrent, optimal DC maturation and production of proinflammatory chemokines and pro-Th1 cytokines, such as IL-6, IL-8, IL-12, IFN-, and TNF-. These activated DCs were the most potent cells to support the growth of CD8+, IFN--producing T cells, and to process tumor Ag for the generation of specific cytotoxic T cells in vitro. Animals vaccinated with irradiated CD40L-tumor cell-pulsed DCs were better protected against subsequent challenge of a weakly immunogenic tumor cell line than animals vaccinated with irradiated CD40L-tumor cells alone. Thus, our results strongly support the future clinical application of using DCs pulsed with irradiated CD40L-tumor cells as a cancer vaccine.
机译:为了提高基于肿瘤细胞和基于树突状细胞(DC)的癌症疫苗的功效,本研究探索了一种新的癌症疫苗策略的潜力,即将CD40配体转染的肿瘤(CD40L-tumor)细胞用于同时将肿瘤来源的抗原(Ag)和成熟刺激物传递给DC。共孵育后,未成熟的DC有效地将来自冷冻/融化或辐射的人类肿瘤细胞的材料(具有或不具有表面CD40L)有效地内化。但是,在内部化过程中,仅与经辐照的CD40L肿瘤细胞共培养才能导致同时,最佳的DC成熟并产生促炎性趋化因子和促Th1因子,例如IL-6,IL-8,IL-12,IFN-,和TNF-。这些活化的DC是最强大的细胞,可支持CD8 +和产生IFN的T细胞的生长,并能处理肿瘤Ag以在体外产生特定的细胞毒性T细胞。接种了CD40L肿瘤细胞脉冲辐照的DC的动物比单独接种CD40L肿瘤细胞的动物受到更好的保护,以抵抗免疫原性较弱的肿瘤细胞系的后续攻击。因此,我们的结果有力地支持了将经辐照的CD40L肿瘤细胞脉冲刺激的DC用作癌症疫苗的未来临床应用。

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