PD-1 expression on mouse intratumoral NK cells and its effects on NK cell phenotype

Arnika K. Wagner; Nadir Kadri; Chris Tibbitt; Koen van de Ven; Sunitha Bagawath-Singh; Denys Oliinyk; Eric LeGresley; Nicole Campbell; Stephanie Trittel; Peggy Riese; Ulf Ribacke; Tatyana Sandalova; Adnane Achour; Klas Kärre; Benedict J. Chambers

doi:10.1016/j.isci.2022.105137

PD-1 expression on mouse intratumoral NK cells and its effects on NK cell phenotype

Arnika K. Wagner, Nadir Kadri, Chris Tibbitt, Koen van de Ven, Sunitha Bagawath-Singh, Denys Oliinyk, Eric LeGresley, Nicole Campbell, Stephanie Trittel, Peggy Riese, Ulf Ribacke, Tatyana Sandalova, Adnane Achour, Klas Kärre, Benedict J. Chambers

Research output: Contribution to journal › Article › Research › peer-review

9 Citations (Scopus)

Abstract

Although PD-1 was shown to be a hallmark of T cells exhaustion, controversial studies have been reported on the role of PD-1 on NK cells. Here, we found by flow cytometry and single cell RNA sequencing analysis that PD-1 can be expressed on MHC class I-deficient tumor-infiltrating NK cells in vivo. We also demonstrate distinct alterations in the phenotype of PD-1-deficient NK cells and a more mature phenotype which might reduce their capacity to migrate and kill in vivo. Tumor-infiltrating NK cells that express PD-1 were highly associated with the expression of CXCR6. Furthermore, our results demonstrate that PD-L1 molecules in membranes of PD-1-deficient NK cells migrate faster than in NK cells from wild-type mice, suggesting that PD-1 and PD-L1 form cis interactions with each other on NK cells. These data demonstrate that there may be a role for the PD-1/PD-L1 axis in tumor-infiltrating NK cells in vivo.

Original language	English
Article number	105137
Number of pages	22
Journal	iScience
Volume	25
Issue number	10
DOIs	https://doi.org/10.1016/j.isci.2022.105137
Publication status	Published - 21 Oct 2022
Externally published	Yes

Keywords

Cancer
Components of the immune system
Immunology
Transcriptomics

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.isci.2022.105137Licence: CC BY

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Wagner, A. K., Kadri, N., Tibbitt, C., van de Ven, K., Bagawath-Singh, S., Oliinyk, D., LeGresley, E., Campbell, N., Trittel, S., Riese, P., Ribacke, U., Sandalova, T., Achour, A., Kärre, K., & Chambers, B. J. (2022). PD-1 expression on mouse intratumoral NK cells and its effects on NK cell phenotype. iScience, 25(10), Article 105137. https://doi.org/10.1016/j.isci.2022.105137

@article{33219ea26aa74c5fa7b071dbbaa4258f,

title = "PD-1 expression on mouse intratumoral NK cells and its effects on NK cell phenotype",

abstract = "Although PD-1 was shown to be a hallmark of T cells exhaustion, controversial studies have been reported on the role of PD-1 on NK cells. Here, we found by flow cytometry and single cell RNA sequencing analysis that PD-1 can be expressed on MHC class I-deficient tumor-infiltrating NK cells in vivo. We also demonstrate distinct alterations in the phenotype of PD-1-deficient NK cells and a more mature phenotype which might reduce their capacity to migrate and kill in vivo. Tumor-infiltrating NK cells that express PD-1 were highly associated with the expression of CXCR6. Furthermore, our results demonstrate that PD-L1 molecules in membranes of PD-1-deficient NK cells migrate faster than in NK cells from wild-type mice, suggesting that PD-1 and PD-L1 form cis interactions with each other on NK cells. These data demonstrate that there may be a role for the PD-1/PD-L1 axis in tumor-infiltrating NK cells in vivo.",

keywords = "Cancer, Components of the immune system, Immunology, Transcriptomics",

author = "Wagner, {Arnika K.} and Nadir Kadri and Chris Tibbitt and {van de Ven}, Koen and Sunitha Bagawath-Singh and Denys Oliinyk and Eric LeGresley and Nicole Campbell and Stephanie Trittel and Peggy Riese and Ulf Ribacke and Tatyana Sandalova and Adnane Achour and Klas K{\"a}rre and Chambers, {Benedict J.}",

note = "Funding Information: This work was funded by the Swedish Cancer Society , Swedish Research Council . ScRNA-seq was performed at the eukaryotic single-cell genomics facility at SciLife laboratories (Stockholm, Sweden). The data handling was enabled by resources provided by the Swedish National Infrastructure for Computing (SNIC) at Uppsala partially funded by the Swedish Research Council through grant agreement no. 2018-05973 . We also thank Jonas S{\o}ndergaard for advice regarding the scRNA-seq analyses. The graphical abstract was created with BioRender.com . Publisher Copyright: {\textcopyright} 2022 The Author(s)",

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doi = "10.1016/j.isci.2022.105137",

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T1 - PD-1 expression on mouse intratumoral NK cells and its effects on NK cell phenotype

AU - Wagner, Arnika K.

AU - Kadri, Nadir

AU - Tibbitt, Chris

AU - van de Ven, Koen

AU - Bagawath-Singh, Sunitha

AU - Oliinyk, Denys

AU - LeGresley, Eric

AU - Campbell, Nicole

AU - Trittel, Stephanie

AU - Riese, Peggy

AU - Ribacke, Ulf

AU - Sandalova, Tatyana

AU - Achour, Adnane

AU - Kärre, Klas

AU - Chambers, Benedict J.

N1 - Funding Information: This work was funded by the Swedish Cancer Society , Swedish Research Council . ScRNA-seq was performed at the eukaryotic single-cell genomics facility at SciLife laboratories (Stockholm, Sweden). The data handling was enabled by resources provided by the Swedish National Infrastructure for Computing (SNIC) at Uppsala partially funded by the Swedish Research Council through grant agreement no. 2018-05973 . We also thank Jonas Søndergaard for advice regarding the scRNA-seq analyses. The graphical abstract was created with BioRender.com . Publisher Copyright: © 2022 The Author(s)

PY - 2022/10/21

Y1 - 2022/10/21

N2 - Although PD-1 was shown to be a hallmark of T cells exhaustion, controversial studies have been reported on the role of PD-1 on NK cells. Here, we found by flow cytometry and single cell RNA sequencing analysis that PD-1 can be expressed on MHC class I-deficient tumor-infiltrating NK cells in vivo. We also demonstrate distinct alterations in the phenotype of PD-1-deficient NK cells and a more mature phenotype which might reduce their capacity to migrate and kill in vivo. Tumor-infiltrating NK cells that express PD-1 were highly associated with the expression of CXCR6. Furthermore, our results demonstrate that PD-L1 molecules in membranes of PD-1-deficient NK cells migrate faster than in NK cells from wild-type mice, suggesting that PD-1 and PD-L1 form cis interactions with each other on NK cells. These data demonstrate that there may be a role for the PD-1/PD-L1 axis in tumor-infiltrating NK cells in vivo.

AB - Although PD-1 was shown to be a hallmark of T cells exhaustion, controversial studies have been reported on the role of PD-1 on NK cells. Here, we found by flow cytometry and single cell RNA sequencing analysis that PD-1 can be expressed on MHC class I-deficient tumor-infiltrating NK cells in vivo. We also demonstrate distinct alterations in the phenotype of PD-1-deficient NK cells and a more mature phenotype which might reduce their capacity to migrate and kill in vivo. Tumor-infiltrating NK cells that express PD-1 were highly associated with the expression of CXCR6. Furthermore, our results demonstrate that PD-L1 molecules in membranes of PD-1-deficient NK cells migrate faster than in NK cells from wild-type mice, suggesting that PD-1 and PD-L1 form cis interactions with each other on NK cells. These data demonstrate that there may be a role for the PD-1/PD-L1 axis in tumor-infiltrating NK cells in vivo.

KW - Cancer

KW - Components of the immune system

KW - Immunology

KW - Transcriptomics

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SN - 2589-0042

VL - 25

JO - iScience

JF - iScience

IS - 10

M1 - 105137

ER -

PD-1 expression on mouse intratumoral NK cells and its effects on NK cell phenotype

Abstract

Keywords

UN SDGs

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