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Tn 糖基化修饰 MUC6 蛋白可调节其免疫原性,并促进 Th17 偏向性 T 细胞应答的诱导。

Tn glycosylation of the MUC6 protein modulates its immunogenicity and promotes the induction of Th17-biased T cell responses.

机构信息

From the Institut Pasteur, Department of Immunology, Immune Regulation and Vaccinology Unit, 75015 Paris,; INSERM, U1041, Paris,; the Institut Pasteur, Département de Biologie Structurale et Chimie, Unité de Chimie des Biomolécules, 75015 Paris, and; the CNRS, URA 2128, Paris, France.

From the Institut Pasteur, Department of Immunology, Immune Regulation and Vaccinology Unit, 75015 Paris,; INSERM, U1041, Paris.

出版信息

J Biol Chem. 2011 Mar 11;286(10):7797-7811. doi: 10.1074/jbc.M110.209742. Epub 2010 Dec 30.

Abstract

The Tn antigen (α-GalNAc-O-Ser/Thr) is one of the most specific human cancer-associated structures. This antigen, together with mucins, the major carriers of O-glycosylated tumor antigens in adenocarcinomas, are being evaluated as anti-cancer immunotherapeutic targets. In particular, the MUC6 protein, which is normally expressed only in gastric tissues, has been detected in intestinal, pulmonary, colorectal, and breast carcinomas. To develop anti-cancer vaccines based on the Tn antigen, we produced MUC6 proteins with different Tn density by using mixtures of recombinant ppGalNAc-T1, -T2, and -T7. The obtained glycoproteins were characterized and analyzed for their immunological properties, as compared with the non-glycosylated MUC6. We show that these various MUC6:Tn glycoproteins were well recognized by both MUC6 and Tn-specific antibodies. However, Tn glycosylation of the MUC6 protein strongly affected their immunogenicity by partially abrogating Th1 cell responses, and promoting IL-17 responses. Moreover, the non-glycosylated MUC6 was more efficiently presented than MUC6:Tn glycoproteins to specific T CD4(+) hybridomas, suggesting that Tn glycosylation may affect MUC6 processing or MHC binding of the processed peptides. In conclusion, our results indicate that Tn glycosylation of the MUC6 protein strongly affects its B and T cell immunogenicity, and might favor immune escape of tumor cells.

摘要

Tn 抗原(α-GalNAc-O-Ser/Thr)是最具特异性的人类癌症相关结构之一。这种抗原与粘蛋白一起,作为腺癌中 O-糖基化肿瘤抗原的主要载体,正在被评估为抗癌免疫治疗靶点。特别是,正常仅在胃组织中表达的 MUC6 蛋白已在肠、肺、结直肠和乳腺癌中被检测到。为了基于 Tn 抗原开发抗癌疫苗,我们使用重组 ppGalNAc-T1、-T2 和 -T7 的混合物生产了具有不同 Tn 密度的 MUC6 蛋白。对获得的糖蛋白进行了表征和分析,以比较其免疫原性与非糖基化的 MUC6。我们表明,这些不同的 MUC6:Tn 糖蛋白都被 MUC6 和 Tn 特异性抗体很好地识别。然而,MUC6 蛋白的 Tn 糖基化通过部分消除 Th1 细胞反应和促进 IL-17 反应强烈影响其免疫原性。此外,与 MUC6:Tn 糖蛋白相比,非糖基化的 MUC6 更有效地呈递给特异性 T CD4(+)杂交瘤,这表明 Tn 糖基化可能影响 MUC6 的加工或加工肽与 MHC 的结合。总之,我们的结果表明,MUC6 蛋白的 Tn 糖基化强烈影响其 B 和 T 细胞免疫原性,并可能有利于肿瘤细胞的免疫逃逸。

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