IFI35 limits antitumor immunity in triple-negative breast cancer via CCL2 secretion.
Baojin XuHefen SunSimeng LiuLi LiaoXiaoqing SongYi WuYifeng HouWei JinPublished in: Oncogene (2024)
Triple-negative breast cancer (TNBC) is the most aggressive subtype of breast cancer with poor prognosis due to the lack of therapeutic targets. Although immunotherapy brings survival benefits to patients diagnosed with TNBC, it remains limited and treatment resistance is widespread. Here we demonstrate that IFI35 is highly expressed in tumor tissues and can be induced by Interferon-γ in a time-dependent and concentration-dependent manner in breast cancer cells. In xenograft models, we reveal that IFI35 dramatically increases myeloid-derived suppressor cells infiltration in tumors, along with depletion and anergy of CD8 + T cells. IFI35 ablation leads to prolonged survival of the mice. Mechanistically, RNA-sequencing reveals that IFI35 promotes CCL2 secretion, resulting in the remodeling of TNBC immune microenvironment. Ablation of IFI35 promotes the infiltration of effector CD8 + T cells, and thereby sensitizes TNBC to anti-PD-1 immunotherapy. Our data suggest that IFI35 limits antitumor immunity and may be expected to become a new immunotherapy target in TNBC.
Keyphrases
- poor prognosis
- induced apoptosis
- end stage renal disease
- long non coding rna
- single cell
- breast cancer cells
- dendritic cells
- chronic kidney disease
- stem cells
- ejection fraction
- newly diagnosed
- genome wide
- skeletal muscle
- metabolic syndrome
- liver fibrosis
- cell proliferation
- liver injury
- peritoneal dialysis
- cell death
- cell cycle arrest
- big data
- young adults
- high fat diet induced
- radiofrequency ablation
- drug induced
- atrial fibrillation
- catheter ablation
- type iii
- data analysis