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Tumor-infiltrating mucosal-associated invariant T (MAIT) cells retain expression of cytotoxic effector molecules

机译:肿瘤浸润性黏膜相关不变T(MAIT)细胞保留细胞毒性效应分子的表达

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摘要

Mucosal-associated invariant T (MAIT) cells all express a semi-invariable T cell receptor recognizing microbial metabolites presented on the MHC class I-like molecule MR1. Upon activation, they rapidly secrete cytokines and increase their cytotoxic potential. We showed recently that MAIT cells with Th1 phenotype accumulate in human colon adenocarcinomas. Here, we investigated the cytotoxic potential of tumor-infiltrating MAIT cells in colon adenocarcinomas, and to what extent it may be affected by the tumor microenvironment. Activation of MAIT cells from tumors induced increased Granzyme B, and to a lesser extent, perforin expression. Degranulation was assessed by surface expression of CD107a, and was also seen in response to cognate antigen recognition. The cytotoxic potential of tumor-associated MAIT cells was very similar to that of MAIT cells from unaffected colon. MAIT cells were also identified by immunofluorescence in direct contact with tumor cells in sections from colon cancer specimens. To summarize, tumor-associated MAIT cells from colon tumors have strong cytotoxic potential and are not compromised in this regard compared to MAIT cells from the unaffected colon. We conclude that MAIT cells may contribute significantly to the protective immune response to tumors, both by secretion of Th1-associated cytokines and by direct killing of tumor cells.
机译:粘膜相关不变T(MAIT)细胞均表达识别MHC I类分子MR1上呈现的微生物代谢产物的半不变T细胞受体。激活后,它们会迅速分泌细胞因子并增加其细胞毒性潜力。我们最近显示,具有Th1表型的MAIT细胞在人结肠腺癌中积累。在这里,我们研究了肿瘤浸润的MAIT细胞在结肠腺癌中的细胞毒性潜力,以及它在多大程度上可能受肿瘤微环境的影响。来自肿瘤的MAIT细胞的活化诱导了颗粒酶B的增加,并在较小程度上促进了穿孔素的表达。通过CD107a的表面表达评估脱粒,并且还可以观察到对同源抗原识别的反应。肿瘤相关的MAIT细胞的细胞毒性潜力与未受影响的结肠的MAIT细胞非常相似。在与结肠癌标本切片中的肿瘤细胞直接接触时,还通过免疫荧光鉴定了MAIT细胞。总之,与来自未受影响结肠的MAIT细胞相比,来自结肠肿瘤的肿瘤相关MAIT细胞具有很强的细胞毒性潜能,并且在这方面没有受到损害。我们得出的结论是,MAIT细胞可能通过分泌与Th1相关的细胞因子和直接杀死肿瘤细胞而大大促进了对肿瘤的保护性免疫应答。

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