Monocytes reprogrammed by tumor microparticle vaccine inhibit tumorigenesis and tumor development

被引:0
作者
Weiwei Sun
Lili Dai
Yuqing Cao
Pengtao Pan
Lijuan Zhi
Xinke Wang
Xinzhong Yuan
Zi Gao
Sheng Guo
Guoyan Liu
Junlei Yin
Liangliang Xie
Liping Wang
Yanling Wang
Wensheng Li
Hong Li
Yunjie Jia
机构
[1] Xinxiang University,School of Medicine
[2] Xinxiang Medical University,Department of Immunology, School of Basic Medical Sciences
来源
Cancer Nanotechnology | 2023年 / 14卷
关键词
Tumor microparticles; Monocytes; Monocyte-derived DCs; IRF4; Tumor vaccine;
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摘要
Tumor microparticles (T-MPs) are considered as a tumor vaccine candidate. Although some studies have analyzed the mechanism of T-MPs as tumor vaccine, we still lack understanding of how T-MPs stimulate a strong anti-tumor immune response. Here, we show that T-MPs induce macrophages to release a key chemotactic factor CCL2, which attracts monocytes to the vaccine injection site and enhances endocytosis of antigen. Monocytes subsequently enter the draining lymph node, and differentiate into monocyte-derived DCs (moDCs), which present tumor antigens to T lymphocytes and deliver a potent anti-tumor immune response. Mechanically, T-MPs activate the cGAS-STING signaling through DNA fragments, and then induce monocytes to upregulate the expression of IRF4, which is a key factor for monocyte differentiation into moDCs. More importantly, monocytes that have endocytosed T-MPs acquire the ability to treat tumors. Collectively, this work might provide novel vaccination strategy for the development of tumor vaccines and facilitate the application of T-MPs for clinic oncotherapy.
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