利用基于邻近性的排序酶 A 介导的 T 细胞表位连接技术开发靶向抗原呈递细胞的多功能癌症疫苗形式

IF 4 2区 化学 Q1 BIOCHEMICAL RESEARCH METHODS
Aru Z. Wang, Hendrik J. Brink, Rianne G. Bouma, Alsya J. Affandi, Maarten K. Nijen Twilhaar, Dijmphna A. M. Heijnen, Joelle van Elk, Janneke J. Maaskant, Veronique A. L. Konijn, Joeke G. C. Stolwijk, Hakan Kalay, Katarina Olesek, Yvette van Kooyk, Johan M. S. van der Schoot, Arthur E. H. Bentlage, Ferenc A. Scheeren, Martijn Verdoes, Gestur Vidarsson, Coenraad P. Kuijl and Joke M. M. den Haan*, 
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引用次数: 0

摘要

癌症疫苗是一种很有前景的策略,可以提高对检查点抑制剂反应不充分的患者的肿瘤特异性免疫反应。含有患者特异性肿瘤抗原的癌症疫苗最为有效,但也需要生产患者特异性疫苗。本研究旨在开发一种多功能癌症疫苗形式,其中患者特异性肿瘤抗原可通过基于接近性的排序酶 A(SrtA)介导的连接(PBSL)方法与抗体特异性结合,从而特异性地结合到抗原递呈细胞上,刺激免疫反应。DEC205和CD169都是抗原递呈细胞上表达的受体,可以靶向递送抗原并刺激T细胞反应。我们利用 CRISPR/HDR 平台制备了具有 DEC205 或 CD169 特异性的小鼠重链 IgG2a 抗体,该抗体含有 SrtA 识别基序,C 端带有 SpyTag。利用与 SpyCatcher 连接的 SrtA 重组蛋白,我们采用基于 SrtA 介导的近距离连接技术将异硫氰酸荧光素(FITC)标记的肽或抗原肽连接到抗体上。连接后的抗体在体外和体内都能与表达 DEC205 的树突状细胞或表达 CD169 的巨噬细胞结合。更重要的是,用与 T 细胞表位相连的 DEC205 或 CD169 特异性抗体进行免疫,能有效激发体内的 T 细胞反应。总之,我们利用 PBSL 开发出了一种癌症疫苗形式,它能快速加入肿瘤抗原,有可能用于合成个性化癌症疫苗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Development of a Versatile Cancer Vaccine Format Targeting Antigen-Presenting Cells Using Proximity-Based Sortase A-Mediated Ligation of T-Cell Epitopes

Cancer vaccines are a promising strategy to increase tumor-specific immune responses in patients who do not adequately respond to checkpoint inhibitors. Cancer vaccines that contain patient-specific tumor antigens are most effective but also necessitate the production of patient-specific vaccines. This study aims to develop a versatile cancer vaccine format in which patient-specific tumor antigens can be site-specifically conjugated by a proximity-based Sortase A (SrtA)-mediated ligation (PBSL) approach to antibodies that specifically bind to antigen-presenting cells to stimulate immune responses. DEC205 and CD169 are both receptors expressed on antigen-presenting cells that can be targeted to deliver antigens and stimulate T-cell responses. We used the CRISPR/HDR platform to produce mouse heavy chain IgG2a antibodies with DEC205 or CD169 specificity containing an SrtA recognition motif followed by a SpyTag at the C-terminus. Using a recombinant protein of SrtA linked to SpyCatcher, we applied proximity-based SrtA-mediated ligation to ligate fluorescein isothiocyanate (FITC)-labeled or antigenic peptides to the antibodies. Ligated antibodies bound to DEC205-expressing dendritic cells or CD169-expressing macrophages both in vitro and in vivo. More importantly, immunization with DEC205- or CD169-specific Abs linked to T-cell epitopes efficiently stimulated T-cell responses in vivo. To conclude, we have developed a cancer vaccine format using PBSL that enables the rapid incorporation of tumor antigens and could potentially be implemented for the synthesis of personalized cancer vaccines.

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来源期刊
Bioconjugate Chemistry
Bioconjugate Chemistry 生物-化学综合
CiteScore
9.00
自引率
2.10%
发文量
236
审稿时长
1.4 months
期刊介绍: Bioconjugate Chemistry invites original contributions on all research at the interface between man-made and biological materials. The mission of the journal is to communicate to advances in fields including therapeutic delivery, imaging, bionanotechnology, and synthetic biology. Bioconjugate Chemistry is intended to provide a forum for presentation of research relevant to all aspects of bioconjugates, including the preparation, properties and applications of biomolecular conjugates.
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