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Effective antigen cross-presentation by prostate cancer patients' dendritic cells: implications for prostate cancer immunotherapy

机译:前列腺癌患者树突状细胞的有效抗原交叉呈递:对前列腺癌免疫疗法的意义

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Despite the potency with which dendritic cells (DCs) are able to utilize the exogenous MHC I antigen cross-presentation pathway to cross-present antigen for the activation of killer T cells in model systems, concern about defects in immune function in cancer patients has led to uncertainty regarding whether immune cells derived from patients can effectively be used to generate tumor vaccines. We have undertaken a careful analysis of the potency of using DCs obtained from prostate cancer patients to cross-present antigen derived from human prostate tumor cells for the activation of antigen-specific T cells. Such DCs can be matured ex vivo into functionally active cells and are capable of cross-presenting influenza antigen derived from internalized apoptotic prostate tumor cells. Importantly, we demonstrate effective stimulation of both CD4+ and CD8+ T cells, as evident by production of IFN-, and the ability of CD8+ T cells to differentiate into effector CTLs. These results, defining conditions in which prostate cancer patient DCs can efficiently utilize the cross-presentation pathway and in which apoptotic tumor can serve as a source of antigen for DCs to activate T cells, demonstrate that this system warrants clinical study as a potential immunotherapy.
机译:尽管树突状细胞(DC)能够利用外源性MHC I抗原交叉呈递途径交叉呈递抗原以激活模型系统中的杀伤性T细胞,但对癌症患者免疫功能缺陷的担忧导致关于源自患者的免疫细胞是否可以有效用于产生肿瘤疫苗的不确定性。我们对使用从前列腺癌患者获得的DC交叉呈递源自人前列腺肿瘤细胞的抗原来激活抗原特异性T细胞的能力进行了仔细的分析。这样的DC可以离体成熟成功能活跃的细胞,并且能够交叉呈递源自内在化的凋亡前列腺肿瘤细胞的流感抗原。重要的是,我们证明了对CD4 +和CD8 + T细胞的有效刺激,这可以通过产生IFN-以及CD8 + T细胞分化为效应CTL的能力来证明。这些结果定义了前列腺癌患者DC可以有效利用交叉呈递途径以及凋亡性肿瘤可以作为DC激活T细胞的抗原来源的条件,这些结果证明该系统值得临床研究作为潜在的免疫疗法。

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