The CCR2/MCP-1 Chemokine Pathway and Lung Adenocarcinoma.
Payal MittalLiqing WangTatiana AkimovaCraig A LeachJose C ClementeMatthew R SenderYao ChenBrandon J TurunenWayne W HancockPublished in: Cancers (2020)
Host anti-tumor immunity can be hindered by various mechanisms present within the tumor microenvironment, including the actions of myeloid-derived suppressor cells (MDSCs). We investigated the role of the CCR2/MCP-1 pathway in MDSC-associated tumor progression in murine lung cancer models. Phenotypic profiling revealed maximal expression of CCR2 by tumor-resident MDSCs, and MCP-1 by transplanted TC1 tumor cells, respectively. Use of CCR2-knockout (CCR2-KO) mice showed dependence of tumor growth on CCR2 signaling. Tumors in CCR2-KO mice had fewer CCR2low MDSCs, CD4 T cells and Tregs than WT mice, and increased infiltration by CD8 T cells producing IFN-γ and granzyme-B. Effects were MDSC specific, since WT and CCR2-KO conventional T (Tcon) cells had comparable proliferation and production of inflammatory cytokines, and suppressive functions of WT and CCR2-KO Foxp3+ Treg cells were also similar. We used a thioglycolate-induced peritonitis model to demonstrate a role for CCR2/MCP-1 in trafficking of CCR2+ cells to an inflammatory site, and showed the ability of a CCR2 antagonist to inhibit such trafficking. Use of this CCR2 antagonist promoted anti-tumor immunity and limited tumor growth. In summary, tumor cells are the prime source of MCP-1 that promotes MDSC recruitment, and our genetic and pharmacologic data demonstrate that CCR2 targeting may be an important component of cancer immunotherapy.
Keyphrases
- regulatory t cells
- dendritic cells
- induced apoptosis
- cell cycle arrest
- immune response
- single cell
- type diabetes
- machine learning
- blood pressure
- oxidative stress
- gene expression
- high resolution
- long non coding rna
- endothelial cells
- skeletal muscle
- dna methylation
- patient safety
- big data
- single molecule
- emergency medicine