PD-L1 on tumor cells is sufficient for immune evasion in immunogenic tumors and inhibits CD8 T cell cytotoxicity.
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Abstract | It is unclear whether PD-L1 on tumor cells is sufficient for tumor immune evasion or simply correlates with an inflamed tumor microenvironment. We used three mouse tumor models sensitive to PD-1 blockade to evaluate the significance of PD-L1 on tumor versus nontumor cells. PD-L1 on nontumor cells is critical for inhibiting antitumor immunity in B16 melanoma and a genetically engineered melanoma. In contrast, PD-L1 on MC38 colorectal adenocarcinoma cells is sufficient to suppress antitumor immunity, as deletion of PD-L1 on highly immunogenic MC38 tumor cells allows effective antitumor immunity. MC38-derived PD-L1 potently inhibited CD8(+) T cell cytotoxicity. Wild-type MC38 cells outcompeted PD-L1-deleted MC38 cells in vivo, demonstrating tumor PD-L1 confers a selective advantage. Thus, both tumor- and host-derived PD-L1 can play critical roles in immunosuppression. Differences in tumor immunogenicity appear to underlie their relative importance. Our findings establish reduced cytotoxicity as a key mechanism by which tumor PD-L1 suppresses antitumor immunity and demonstrate that tumor PD-L1 is not just a marker of suppressed antitumor immunity. |
Year of Publication | 2017
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Journal | J Exp Med
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Volume | 214
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Issue | 4
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Pages | 895-904
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Date Published | 2017 Apr 03
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ISSN | 1540-9538
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DOI | 10.1084/jem.20160801
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PubMed ID | 28302645
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PubMed Central ID | PMC5379970
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Grant list | P01 AI056299 / AI / NIAID NIH HHS / United States
P50 CA101942 / CA / NCI NIH HHS / United States
R01 AI040614 / AI / NIAID NIH HHS / United States
U54 CA163125 / CA / NCI NIH HHS / United States
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