Blockade of surface-bound TGF-β on regulatory T cells abrogates suppression of effector T cell function in the tumor microenvironment.
Sadna BudhuDavid A SchaerYongbiao LiRicardo Toledo-CrowKatherine PanageasXia YangHong ZhongAlan N HoughtonSamuel C SilversteinTaha MerghoubJedd D WolchokPublished in: Science signaling (2017)
Regulatory T cells (Tregs) suppress antitumor immunity by inhibiting the killing of tumor cells by antigen-specific CD8+ T cells. To better understand the mechanisms involved, we used ex vivo three-dimensional collagen-fibrin gel cultures of dissociated B16 melanoma tumors. This system recapitulated the in vivo suppression of antimelanoma immunity, rendering the dissociated tumor cells resistant to killing by cocultured activated, antigen-specific T cells. Immunosuppression was not observed when tumors excised from Treg-depleted mice were cultured in this system. Experiments with neutralizing antibodies showed that blocking transforming growth factor-β (TGF-β) also prevented immunosuppression. Immunosuppression depended on cell-cell contact or cellular proximity because soluble factors from the collagen-fibrin gel cultures did not inhibit tumor cell killing by T cells. Moreover, intravital, two-photon microscopy showed that tumor-specific Pmel-1 effector T cells physically interacted with tumor-resident Tregs in mice. Tregs isolated from B16 tumors alone were sufficient to suppress CD8+ T cell-mediated killing, which depended on surface-bound TGF-β on the Tregs Immunosuppression of CD8+ T cells correlated with a decrease in the abundance of the cytolytic protein granzyme B and an increase in the cell surface amount of the immune checkpoint receptor programmed cell death protein 1 (PD-1). These findings suggest that contact between Tregs and antitumor T cells in the tumor microenvironment inhibits antimelanoma immunity in a TGF-β-dependent manner and highlight potential ways to inhibit intratumoral Tregs therapeutically.
Keyphrases
- regulatory t cells
- transforming growth factor
- dendritic cells
- epithelial mesenchymal transition
- single cell
- cell therapy
- cell surface
- high resolution
- signaling pathway
- binding protein
- type diabetes
- immune response
- protein protein
- microbial community
- bone marrow
- skeletal muscle
- adipose tissue
- mesenchymal stem cells
- zika virus
- risk assessment
- living cells
- optical coherence tomography
- climate change
- insulin resistance
- aedes aegypti
- dengue virus
- platelet rich plasma