Contribution of NK cells to immunotherapy mediated by PD-1/PD-L1 blockade
Joy Hsu, … , David H. Raulet, Michele Ardolino
Joy Hsu, … , David H. Raulet, Michele Ardolino
Published September 10, 2018
Citation Information: J Clin Invest. 2018;128(10):4654-4668. https://doi.org/10.1172/JCI99317.
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Contribution of NK cells to immunotherapy mediated by PD-1/PD-L1 blockade

Abstract

Checkpoint blockade immunotherapy targeting the PD-1/PD-L1 inhibitory axis has produced remarkable results in the treatment of several types of cancer. Whereas cytotoxic T cells are known to provide important antitumor effects during checkpoint blockade, certain cancers with low MHC expression are responsive to therapy, suggesting that other immune cell types may also play a role. Here, we employed several mouse models of cancer to investigate the effect of PD-1/PD-L1 blockade on NK cells, a population of cytotoxic innate lymphocytes that also mediate antitumor immunity. We discovered that PD-1 and PD-L1 blockade elicited a strong NK cell response that was indispensable for the full therapeutic effect of immunotherapy. PD-1 was expressed on NK cells within transplantable, spontaneous, and genetically induced mouse tumor models, and PD-L1 expression in cancer cells resulted in reduced NK cell responses and generation of more aggressive tumors in vivo. PD-1 expression was more abundant on NK cells with an activated and more responsive phenotype and did not mark NK cells with an exhausted phenotype. These results demonstrate the importance of the PD-1/PD-L1 axis in inhibiting NK cell responses in vivo and reveal that NK cells, in addition to T cells, mediate the effect of PD-1/PD-L1 blockade immunotherapy.

Authors

Joy Hsu, Jonathan J. Hodgins, Malvika Marathe, Chris J. Nicolai, Marie-Claude Bourgeois-Daigneault, Troy N. Trevino, Camillia S. Azimi, Amit K. Scheer, Haley E. Randolph, Thornton W. Thompson, Lily Zhang, Alexandre Iannello, Nikhita Mathur, Karen E. Jardine, Georgia A. Kirn, John C. Bell, Michael W. McBurney, David H. Raulet, Michele Ardolino

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Figure 8

PD-1 is upregulated on the most activated tumor-infiltrating NK cells.

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PD-1 is upregulated on the most activated tumor-infiltrating NK cells. (...
(A) PD-1 expression on different NK cell maturation subsets in RMA-S tumors. R0–R3 stages are as follows: R0, CD27CD11b; R1, CD27+CD11b; R2, CD27+CD11b+; R3, CD27CD11b+. Three independent experiments were pooled (n = 7–18/combined group). One-way ANOVA with repeated measures. *P < 0.05; ***P < 0.001. (B) NK cells from RMA-S tumors were stained with antibodies for Ly49I (I), Ly49C (C), and NKG2A (N), and PD-1 expression was assessed on the 3 populations by flow cytometry. C+I+N+ cells expressed all the receptors; C+±I+±N+ cells expressed at least 1 of the receptors; CIN NK cells lacked expression of all 3 receptors. Data from 2 independent experiments are included. One-way ANOVA with repeated measures. NK cells from RMA-S (C), CT26 (D), or KP sarcoma (E) tumors were costained with PD-1 antibody and antibody against Sca-1 or CD69. PD-1 expression was assessed by flow cytometry on gated NK cells that did or did not express such markers. Representative contour plots and summary of the data are depicted. For C and E, 3 independent experiments were pooled; for D, 2 independent experiments were pooled. n = 6–15. Two-tailed paired Student’s t test.