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OX40L enhances the immunogenicity of dendritic cells and inhibits tumor metastasis in mice

免疫系统 生物 体内 免疫原性 树突状细胞 CD8型 免疫疗法 抗原提呈细胞 抗原 抗原呈递 癌症研究 免疫学 交叉展示 获得性免疫系统 细胞生物学 T细胞 生物技术
作者
Lin Zhao,Wenjie Zhang,Meng Li,Ruoyu Jia,Juncheng Wang,Fengge Wang,Yuekang Xu
出处
期刊:Microbiology and Immunology [Wiley]
卷期号:67 (2): 79-89
标识
DOI:10.1111/1348-0421.13037
摘要

A well preserved immune system is a powerful tool to prevent foreign invasion or to suppress internal mutation, which must be tightly controlled by co-stimulatory molecules in different pathophysiological conditions. One such critical molecule is OX40L expressed on activated antigen-presenting cells (APCs). Consistently, its abnormality is associated with various immunological disorders such as autoinflammatory diseases and allergy. However, a comprehensive analysis of the immune-moderating role of OX40L in dendritic cells (DCs), the most powerful APCs to initiate immune responses in vivo, and investigation of its anti-tumor efficacy in the disease setting have not been performed properly. In this study, genetic approaches for both gain-of-function and reduction-of-function were employed to reveal that OX40L was required for the efficient presentation, but not uptake, of antigens by DCs to stimulate CD4+ , as well as CD8+ T cells in vivo. As a result, CD4+ T cells were promoted towards Th1, but inhibited on Treg differentiation, by the LPS-induced OX40L on DCs, which was supported by their altered expression of co-inhibitory receptor, PD-L1. CD8+ T cells, on the other hand, also enhanced their cytotoxicity towards target cells in response to OX40L expression on the DCs transferred in vivo. Finally, in a DC-mediated tumor immunity model, the strong immunogenic roles of OX40L on DCs led to better metastasis inhibition in vivo. Collectively, our results demonstrate that OX40L could serve as a potential target in the DC-based vaccine for enhanced anti-tumor efficacy in vivo.
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