DNA-based artificial dendritic cells for in situ cytotoxic T cell stimulation and immunotherapy

被引:7
|
作者
Quoc-Viet Le [1 ,2 ]
Lee, Jaiwoo [1 ,2 ]
Byun, Junho [1 ,2 ]
Shim, Gayong [3 ]
Oh, Yu-Kyoung [1 ,2 ]
机构
[1] Seoul Natl Univ, Coll Pharm, 1 Gwanak Ro, Seoul 08826, South Korea
[2] Seoul Natl Univ, Res Inst Pharmaceut Sci, 1 Gwanak Ro, Seoul 08826, South Korea
[3] Soongsil Univ, Sch Syst Biomed Sci, Seoul 06978, South Korea
基金
新加坡国家研究基金会;
关键词
Artificial dendritic cell; DNA microflower; In situ T cell stimulation; Programmed T cell expansion; Immunotherapy; ANTIGEN-PRESENTING CELLS; EX-VIVO EXPANSION; DESIGN;
D O I
10.1016/j.bioactmat.2021.12.001
中图分类号
R318 [生物医学工程];
学科分类号
0831 ;
摘要
In immunotherapy, ex vivo stimulation of T cells requires significant resources and effort. Here, we report artificial dendritic cell-mimicking DNA microflowers (DM) for programming T cell stimulation in situ. To mimic dendritic cells, DNA-based artificial dendritic microflowers were constructed, surface-coated with polydopamine, and further modified with anti-CD3 and anti-CD28 antibodies to yield antibody-modified DM (DM-A). The porous structure of DM-A allowed entrapment of the T cell-stimulating cytokine, ineterleukin-2, yielding interleukin-2-loaded DM-A (DM-AI). For comparison, polystyrene microparticles coated with polydopamine and modified with anti-CD3 and anti-CD28 antibodies (PS-A) were used. Compared to PS-A, DM-AI showed significantly greater contact with T cell surfaces. DM-AI provided the highest ex vivo expansion of cytotoxic T cells. Local injection of DM-AI to tumor tissues induced the recruitment of T cells and expansion of cytotoxic T cells in tumor microenvironments. Unlike the other groups, model animals injected with DM-AI did not exhibit growth of primary tumors. Treatment of mice with DM-AI also protected against growth of a rechallenged distant tumor, and thus prevented tumor recurrence in this model. DM-AI has great potential for programmed stimulation of CD8(+) T cells. This concept could be broadly extended for the programming of specific T cell stimulation profiles.
引用
收藏
页码:160 / 172
页数:13
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