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首页> 外文期刊>Cancer immunology, immunotherapy : >Antigen loading of DCs with irradiated apoptotic tumor cells induces improved anti-tumor immunity compared to other approaches
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Antigen loading of DCs with irradiated apoptotic tumor cells induces improved anti-tumor immunity compared to other approaches

机译:与其他方法相比,辐射的凋亡肿瘤细胞对抗原的抗原负载可提高抗肿瘤免疫力

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摘要

Dendritic cells (DCs) serve as central regulators of adaptive immunity by presenting antigens and providing necessary co-signals. Environmental information received by the DCs determines the co-signals delivered to the responding adaptive cells and, ultimately, the outcome of the interaction. DCs loaded with relevant antigens have been used as therapeutic cellular vaccines, but the optimal antigen loading method has not been determined. We compared different methods to load class I and class II epitopes from the male antigenic complex, HY, onto DCs for the potency of the immune response induced in vivo. Co-incubation of female DCs with HY peptides, RNA or cell lysate from HY expressing tumor induced immune responses equivalent to male DCs. In contrast, female DCs incubated with irradiated, apoptotic HY expressing tumor cells (or male B cells) generated a stronger immune response than male DCs or female DCs loaded using any of the other methods. DC loading with apoptotic tumor resulted in complete protection against high dose HY-expressing tumor challenge whereas 100% lethality was observed in groups receiving DCs that were loaded with peptides, RNA, or lysate. We conclude that signals provided to the DCs by apoptotic cells substantially augment the potency of DC vaccines.
机译:树突状细胞(DC)通过呈递抗原并提供必要的共信号来充当适应性免疫的中央调节器。 DC接收到的环境信息确定了传递到响应的自适应单元的共信号,并最终确定了交互的结果。负载有相关抗原的DC已被用作治疗性细胞疫苗,但尚未确定最佳的抗原负载方法。我们比较了从雄性抗原复合物HY加载I类和II类表位到DC上的不同方法,以了解体内诱导的免疫应答的效力。将雌性DC与表达肿瘤的HY肽,RNA或细胞裂解物共同孵育,诱导肿瘤的免疫反应与雄性DC相同。相比之下,与辐射的,表达凋亡的HY表达肿瘤细胞(或雄性B细胞)孵育的雌性DC产生的免疫反应比雄性DC或使用其他任何方法加载的雌性DC都强。具有凋亡性肿瘤的DC负载可完全抵御高剂量表达HY的肿瘤攻击,而接受DC且负载有肽,RNA或裂解物的组可观察到100%的致死率。我们得出结论,凋亡细胞提供给DC的信号大大增强了DC疫苗的效力。

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