The expression profiles and regulation of PD-L1 in tumor-induced myeloid-derived suppressor cells

The expression profiles and regulation of PD-L1 in tumor-induced myeloid-derived suppressor cells

Programmed death-ligand 1 (PD-L1) is an inhibitory ligand that binds to PD-1 to suppress T cell activation. PD-L1 is constitutively expressed and inducible in tumor cells, but the expression profiles and regulatory mechanism of PD-L1 in myeloid-derived suppressor cells (MDSCs) are largely unknown. W...

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Veröffentlicht in:Oncoimmunology 2016-12, Vol.5 (12), p.e1247135-e1247135
Hauptverfasser: Lu, Chunwan, Redd, Priscilla S., Lee, Jeffrey R., Savage, Natasha, Liu, Kebin
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Sprache:eng
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IFNγ
MDSCs
MSI colon cancer
MSS colon cancer
Original Research
PD-L1
T cells
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container_issue 12
container_start_page e1247135
container_title Oncoimmunology
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creator Lu, Chunwan
Redd, Priscilla S.
Lee, Jeffrey R.
Savage, Natasha
Liu, Kebin
description Programmed death-ligand 1 (PD-L1) is an inhibitory ligand that binds to PD-1 to suppress T cell activation. PD-L1 is constitutively expressed and inducible in tumor cells, but the expression profiles and regulatory mechanism of PD-L1 in myeloid-derived suppressor cells (MDSCs) are largely unknown. We report that PD-L1 is abundantly expressed in tumor-infiltrating leukocytes in human patients with both microsatellite instable and microsatellite stable colon cancer. About 60% CD11b + CD33 + HLA-DR − MDSCs from peripheral blood of human colon cancer patients are PD-L1 + . PD-L1 + MDSCs are also significantly higher in tumor-bearing mice than in tumor-free mice. Interestingly, the highest PD-L1 + MDSCs were observed in the tumor microenvironment in which 56-71% tumor-infiltrating MDSCs are PD-L1 + in vivo. In contrast, PD-L1 + MDSCs are significantly less in secondary lymphoid organs and peripheral blood as compared to the tumor tissues, whereas bone marrow MDSCs are essentially PD-L1 − in tumor-bearing mice. IFNγ is highly expressed in cells of the tumor tissues and IFNγ neutralization significantly decreased PD-L1 + MDSCs in the tumor microenvironment in vivo. However, IFNγ-activated pSTAT1 does not bind to the cd274 promoter in MDSCs. Instead, pSTAT1 activates expression of IRF1, IRF5, IRF7 and IRF8 in MDSCs, and only pSTAT1-activated IRF1 binds to a unique IRF-binding sequence element in vitro and chromatin in vivo in the cd274 promoter to activate PD-L1 transcription. Our data determine that PD-L1 is highly expressed in tumor-infiltrating MDSCs and in a lesser degree in lymphoid organs, and the pSTAT1-IRF1 axis regulates PD-L1 expression in MDSCs.
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PD-L1 is constitutively expressed and inducible in tumor cells, but the expression profiles and regulatory mechanism of PD-L1 in myeloid-derived suppressor cells (MDSCs) are largely unknown. We report that PD-L1 is abundantly expressed in tumor-infiltrating leukocytes in human patients with both microsatellite instable and microsatellite stable colon cancer. About 60% CD11b + CD33 + HLA-DR − MDSCs from peripheral blood of human colon cancer patients are PD-L1 + . PD-L1 + MDSCs are also significantly higher in tumor-bearing mice than in tumor-free mice. Interestingly, the highest PD-L1 + MDSCs were observed in the tumor microenvironment in which 56-71% tumor-infiltrating MDSCs are PD-L1 + in vivo. In contrast, PD-L1 + MDSCs are significantly less in secondary lymphoid organs and peripheral blood as compared to the tumor tissues, whereas bone marrow MDSCs are essentially PD-L1 − in tumor-bearing mice. IFNγ is highly expressed in cells of the tumor tissues and IFNγ neutralization significantly decreased PD-L1 + MDSCs in the tumor microenvironment in vivo. However, IFNγ-activated pSTAT1 does not bind to the cd274 promoter in MDSCs. Instead, pSTAT1 activates expression of IRF1, IRF5, IRF7 and IRF8 in MDSCs, and only pSTAT1-activated IRF1 binds to a unique IRF-binding sequence element in vitro and chromatin in vivo in the cd274 promoter to activate PD-L1 transcription. 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subjects IFNγ
MDSCs
MSI colon cancer
MSS colon cancer
Original Research
PD-L1
T cells
title The expression profiles and regulation of PD-L1 in tumor-induced myeloid-derived suppressor cells
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