A combination of a TLR7/8 agonist and an epigenetic inhibitor suppresses triple-negative breast cancer through triggering anti-tumor immune

被引：4

作者：

Jiang, Zhenzhen ^{[1
]}

Cai, Guangqing ^{[2
]}

Liu, Haiting ^{[1
]}

Liu, Leping ^{[3
]}

Huang, Rong ^{[1
]}

Nie, Xinmin ^{[1
]}

Gui, Rong ^{[1
]}

Li, Jian ^{[1
]}

Ma, Jinqi ^{[1
]}

Cao, Ke ^{[4
]}

Luo, Yanwei ^{[1
]}

机构：

[1] Cent South Univ, Xiangya Hosp 3, Dept Blood Transfus, Changsha 410013, Hunan, Peoples R China

[2] Changsha Hosp Tradit Chinese Med, Changsha Hosp 8, Dept Orthoped, Changsha 410013, Hunan, Peoples R China

[3] Cent South Univ, Xiangya Hosp 3, Dept Pediat, Changsha 410013, Hunan, Peoples R China

[4] Cent South Univ, Xiangya Hosp 3, Dept Oncol, Changsha 410013, Hunan, Peoples R China

来源：

JOURNAL OF NANOBIOTECHNOLOGY | 2024年 / 22卷 / 01期

关键词：

Triple-negative breast cancer (TNBC); Metal-organic framework; Immunogenic cell death; BET inhibitor; Biomimetic codelivery system; Tumor immune microenvironment; METAL-ORGANIC FRAMEWORKS; IMMUNOGENIC CELL-DEATH; T-CELLS; SELECTIVE-INHIBITION; DENDRITIC CELLS; DRUG-DELIVERY; MEMBRANE; NANOPARTICLES; RECRUITMENT; ENDOCYTOSIS;

D O I：

10.1186/s12951-024-02525-1

中图分类号：

Q81 [生物工程学（生物技术）]; Q93 [微生物学];

学科分类号：

071005 ; 0836 ; 090102 ; 100705 ;

摘要：

Background Combination therapy involving immune checkpoint blockade (ICB) and other drugs is a potential strategy for converting immune-cold tumors into immune-hot tumors to benefit from immunotherapy. To achieve drug synergy, we developed a homologous cancer cell membrane vesicle (CM)-coated metal-organic framework (MOF) nanodelivery platform for the codelivery of a TLR7/8 agonist with an epigenetic inhibitor.Methods A novel biomimetic codelivery system (MCM@UN) was constructed by MOF nanoparticles UiO-66 loading with a bromodomain-containing protein 4 (BRD4) inhibitor and then coated with the membrane vesicles of homologous cancer cells that embedding the 18 C lipid tail of 3M-052 (M). The antitumor immune ability and tumor suppressive effect of MCM@UN were evaluated in a mouse model of triple-negative breast cancer (TNBC) and in vitro. The tumor immune microenvironment was analyzed by multicolor immunofluorescence staining.Results In vitro and in vivo data showed that MCM@UN specifically targeted to TNBC cells and was superior to the free drug in terms of tumor growth inhibition and antitumor immune activity. In terms of mechanism, MCM@UN blocked BRD4 and PD-L1 to prompt dying tumor cells to disintegrate and expose tumor antigens. The disintegrated tumor cells released damage-associated molecular patterns (DAMPs), recruited dendritic cells (DCs) to efficiently activate CD8+ T cells to mediate effective and long-lasting antitumor immunity. In addition, TLR7/8 agonist on MCM@UN enhanced lymphocytes infiltration and immunogenic cell death and decreased regulatory T-cells (Tregs). On clinical specimens, we found that mature DCs infiltrating tumor tissues of TNBC patients were negatively correlated with the expression of BRD4, which was consistent with the result in animal model.Conclusion MCM@UN specifically targeted to TNBC cells and remodeled tumor immune microenvironment to inhibit malignant behaviors of TNBC.

引用

页数：21

共 31 条

[31] Downregulation of miR-182-5p inhibits the proliferation and invasion of triple-negative breast cancer cells through regulating TLR4/NF-κB pathway activity by targeting FBXW7 [J].

Wu, Xingping ;

Chen, Hao ;

Wu, Miantao ;

Peng, Songguo ;

Zhang, Lin .

ANNALS OF TRANSLATIONAL MEDICINE, 2020, 8 (16)

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