前沿:在同源肿瘤模型中,瘤内注射负载抗原的树突状细胞可延迟和逆转 T 细胞耐受。
Cutting edge: delay and reversal of T cell tolerance by intratumoral injection of antigen-loaded dendritic cells in an autochthonous tumor model.
机构信息
Department of Biological Engineering, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.
出版信息
J Immunol. 2010 Jun 1;184(11):5954-8. doi: 10.4049/jimmunol.1000265. Epub 2010 Apr 28.
Abstract
The tumor environment exerts a powerful suppressive influence on infiltrating tumor-reactive T cells. It induces tolerance of adoptively transferred effector T cells as they enter tumors and maintains the tolerance of persisting tumor-infiltrating T cells. In an autochthonous prostate cancer model, in which tumor-reactive CD8 T cells are trackable, we demonstrate that both depletion of endogenous dendritic cells (DCs) and intratumoral injection of Ag-loaded mature DCs delayed the tolerization of tumor-infiltrating effector CD8 T cells. Intratumoral injection of Ag-loaded DCs also reactivated tolerized CD8 T cells in the tumor tissue. The observed effects lasted as long as the injected DCs persisted. These findings are consistent with a critical role of DCs in modulating T cell reactivity in the tumor environment. They also suggest new potential strategies to extend the functionality of transferred effector T cells and to restore function to tolerized tumor-infiltrating T cells for cancer immunotherapy.
摘要
肿瘤微环境对浸润的肿瘤反应性 T 细胞具有强大的抑制作用。它诱导进入肿瘤的过继转移效应 T 细胞耐受,并维持持续浸润肿瘤的 T 细胞的耐受。在一个可追踪肿瘤反应性 CD8 T 细胞的同源前列腺癌模型中,我们证明了耗尽内源性树突状细胞(DCs)和肿瘤内注射负载 Ag 的成熟 DCs 均延迟了浸润肿瘤的效应 CD8 T 细胞的耐受化。肿瘤内注射负载 Ag 的 DCs 也可重新激活肿瘤组织中耐受的 CD8 T 细胞。观察到的效果持续时间与注射的 DC 持续时间一样长。这些发现与 DC 在调节肿瘤微环境中 T 细胞反应性方面的关键作用一致。它们还提示了新的潜在策略,以延长转移效应 T 细胞的功能,并恢复耐受肿瘤浸润 T 细胞的功能,用于癌症免疫治疗。
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