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Synthesis and Immunological Evaluation of a Multicomponent Cancer Vaccine Candidate Containing a Long MUC1 Glycopeptide

机译:含有长MUC1糖肽的多组分癌症疫苗候选物的合成和免疫学评价

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摘要

A fully synthetic MUC1-based cancer vaccine was designed and chemically synthesized containing an endogenous helper T-epitope (MHC class II epitope). The vaccine elicited robust IgG titers that could neutralize cancer cells by antibody-dependent cell-mediated cytotoxicity (ADCC). It also activated cytotoxic T-lymphocytes. Collectively, the immunological data demonstrate engagement of helper T-cells in immune activation. A synthetic methodology was developed for a penta-glycosylated MUC1 glycopeptide, and antisera of mice immunized by the new vaccine recognized such a structure. Previously reported fully synthetic MUC1-based cancer vaccines that elicited potent immune responses employed exogenous helper T-epitopes derived from microbes. It is the expectation that the use of the newly identified endogenous helper T-epitope will be more attractive, because it will activate cognate CD4+ T-cells that will provide critical tumor-specific help intratumorally during the effector stage of tumor rejection and will aid in the generation of sustained immunological memory.
机译:设计并化学合成了一种完全合成的基于MUC1的癌症疫苗,其中包含内源性辅助T表位(MHC II类表位)。该疫苗引发了强大的IgG效价,可以通过抗体依赖性细胞介导的细胞毒性(ADCC)中和癌细胞。它还激活了细胞毒性T淋巴细胞。总体而言,免疫学数据表明辅助性T细胞参与了免疫激活。已开发了一种五糖基化的MUC1糖肽的合成方法,用新疫苗免疫的小鼠的抗血清识别出这种结构。先前报道的完全合成的基于MUC1的癌症疫苗引发有效的免疫反应,使用的是源自微生物的外源性辅助T表位。期望使用新近鉴定的内源性辅助性T表位将更具吸引力,因为它将激活相关的CD4 + T细胞,该CD4 + T细胞将在效应器内在肿瘤内提供关键的肿瘤特异性帮助。肿瘤排斥反应的阶段,将有助于产生持续的免疫记忆。

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