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    題名: 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+ T cells
    作者: (Liu K.-J*)*;(Lu L.-F.);(Cheng H.-T.);(Hung Y.-M.);(Shiou S.-R.);(Whang-Peng J);莊聲宏(Shin-Hun Juang)
    貢獻者: 藥學院藥學系;中國附醫醫學研究部細胞及基因治療研究室
    關鍵詞: dendritic cells;antigen processing;CD40 ligand
    日期: 2004-02
    上傳時間: 2009-08-26 16:34:08 (UTC+8)
    摘要: 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.
    關聯: CANCER GENE THERAPY 11(2)135 ~147
    顯示於類別:[藥學系暨碩博士班] 期刊論文

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