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Critical role of EBNA1-specific CD4+ T cells in the control of mouse Burkitt lymphoma in vivo

机译:EBNA1特异性CD4 + T细胞在体内控制小鼠Burkitt淋巴瘤中的关键作用

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摘要

CD4+ T cells play important roles in orchestrating host immune responses against cancer and infectious diseases. Although EBV-encoded nuclear antigen 1–specific (EBNA1-specific) CD4+ T cells have been implicated in controlling the growth of EBV-associated tumors such as Burkitt lymphoma (BL) in vitro, direct evidence for their in vivo function remains elusive due to the lack of an appropriate experimental BL model. Here, we describe the development of a mouse EBNA1-expressing BL tumor model and the identification of 2 novel MHC H-2I-Ab–restricted T cell epitopes derived from EBNA1. Using our murine BL tumor model and the relevant peptides, we show that vaccination of mice with EBNA1 peptide–loaded DCs can elicit CD4+ T cell responses. These EBNA1-specific CD4+ T cells recognized peptide-pulsed targets as well as EBNA1-expressing tumor cells and were necessary and sufficient for suppressing tumor growth in vivo. By contrast, EBNA1 peptide–reactive CD8+ T cells failed to recognize tumor cells and did not contribute to protective immunity. These studies represent what we believe to be the first demonstration that EBNA1-specific CD4+ T cells can suppress tumor growth in vivo, which suggests that CD4+ T cells play an important role in generating protective immunity against EBV-associated cancer.
机译:CD4 + T细胞在协调宿主针对癌症和传染病的免疫反应中起重要作用。尽管EBV编码的核抗原1特异性(EBNA1特异性)CD4 + T细胞已牵涉体外控制与EBV相关的肿瘤(如伯基特淋巴瘤(BL))的生长,但直接证据表明由于缺乏合适的实验性BL模型,它们的体内功能仍然难以捉摸。在这里,我们描述了小鼠EBNA1表达BL肿瘤模型的发展,以及从EBNA1衍生的2种新型MHC H-2I-A b 限制性T细胞表位的鉴定。使用我们的小鼠BL肿瘤模型和相关肽,我们证明了用EBNA1肽负载的DC接种小鼠可以引起CD4 + T细胞反应。这些EBNA1特异性CD4 + T细胞识别肽脉冲靶标以及表达EBNA1的肿瘤细胞,对于抑制体内肿瘤生长是必要和充分的。相比之下,EBNA1肽反应性CD8 + T细胞无法识别肿瘤细胞,也无助于保护性免疫。这些研究代表了我们认为是第一个证明EBNA1特异性CD4 + T细胞可以在体内抑制肿瘤生长的证据,这表明CD4 + T细胞发挥了重要作用。在产生针对EBV相关癌症的保护性免疫中的作用。

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