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Monocytes reprogrammed by tumor microparticle vaccine inhibit tumorigenesis and tumor development.


ABSTRACT: 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.

Supplementary information

The online version contains supplementary material available at 10.1186/s12645-023-00190-x.

SUBMITTER: Sun W 

PROVIDER: S-EPMC10106871 | biostudies-literature | 2023

REPOSITORIES: biostudies-literature

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Monocytes reprogrammed by tumor microparticle vaccine inhibit tumorigenesis and tumor development.

Sun Weiwei W   Dai Lili L   Cao Yuqing Y   Pan Pengtao P   Zhi Lijuan L   Wang Xinke X   Yuan Xinzhong X   Gao Zi Z   Guo Sheng S   Liu Guoyan G   Yin Junlei J   Xie Liangliang L   Wang Liping L   Wang Yanling Y   Li Wensheng W   Li Hong H   Jia Yunjie Y  

Cancer nanotechnology 20230417 1


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 monocy  ...[more]

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