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基于糖基化 Tn 的疫苗靶向真皮树突状细胞,在没有佐剂的情况下有利于生发中心 B 细胞的发育和产生有效的抗体反应。

Glycosidic Tn-based vaccines targeting dermal dendritic cells favor germinal center B-cell development and potent antibody response in the absence of adjuvant.

机构信息

Immune Regulation and Vaccinology Unit, Department of Immunology, Institut Pasteur, 25-28 Rue du Dr. Roux, Paris Cedex 15, France.

出版信息

Blood. 2010 Nov 4;116(18):3526-36. doi: 10.1182/blood-2010-04-279133. Epub 2010 Aug 18.

DOI:10.1182/blood-2010-04-279133
PMID:20720186
Abstract

In vivo targeting of C-type lectin receptors is an effective strategy for increasing antigen uptake and presentation by dendritic cells (DCs). To induce efficient immune response, glycosylated tumor-associated Tn antigens were used to target DCs through binding to macrophage galactose-type lectin (MGL). The capacity of Tn-glycosylated antigens-and the multiple antigenic glycopeptide Tn3 therapeutic candidate vaccine-to target mouse and human MGL(+) DCs are demonstrated, especially regarding dermal DCs. In mice, MGL(+) CD103(-) dermal DCs efficiently captured and processed glycosylated Tn antigen in vivo, inducing a potent major histocompatibility complex (MHC) class II-restricted T-cell response. Intradermal immunization with Tn-glycopeptides induced high levels of Th2 cytokines-even in the presence of unmethylated cytosine-phosphate-guanosine-and was associated with increased expansion of the germinal center B-cell population. Therefore, MGL acts as an efficient endocytic antigen receptor on dermal DCs in vivo, able to prime Tn-specific T- and B-cell responses. Moreover, even in the absence of adjuvant, immunization with this glycosidic Tn-based vaccine induced high levels of anti-Tn antibody responses, recognizing human tumor cells. In vivo DC-targeting strategies, based on Tn-MGL interactions, constitute a promising strategy for enhancing antigen presentation and inducing potent antibody response.

摘要

在体内靶向 C 型凝集素受体是增加树突状细胞 (DC) 摄取和呈递抗原的有效策略。为了诱导有效的免疫反应,使用糖基化肿瘤相关的 Tn 抗原通过与巨噬细胞半乳糖型凝集素 (MGL) 结合来靶向 DC。已经证明 Tn 糖基化抗原和多抗原糖肽 Tn3 治疗候选疫苗能够靶向小鼠和人 MGL(+)DCs,尤其是皮肤 DCs。在小鼠中,MGL(+)CD103(-)皮肤 DCs 能够有效地在体内捕获和处理糖基化 Tn 抗原,诱导强烈的主要组织相容性复合物 (MHC) 类 II 限制性 T 细胞反应。用 Tn 糖肽进行皮内免疫会诱导高水平的 Th2 细胞因子——即使在未甲基化的胞嘧啶-磷酸-鸟嘌呤存在的情况下——并且与生发中心 B 细胞群体的扩增增加有关。因此,MGL 作为体内皮肤 DC 上有效的内吞抗原受体,能够引发 Tn 特异性 T 细胞和 B 细胞反应。此外,即使没有佐剂,用这种基于糖基化 Tn 的疫苗进行免疫也会诱导高水平的抗 Tn 抗体反应,能够识别人类肿瘤细胞。基于 Tn-MGL 相互作用的体内 DC 靶向策略是增强抗原呈递和诱导有效抗体反应的有前途的策略。

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