Targeting MerTK Enhances Adaptive Immune Responses After Radiation Therapy

Garth W. Tormoen; Tiffany C. Blair; Shelly Bambina; Gwen Kramer; Jason Baird; Ramtin Rahmani; John M. Holland; Owen J.T. McCarty; Michael J. Baine; Vivek Verma; Nima Nabavizadeh; Michael J. Gough; Marka Crittenden

doi:10.1016/j.ijrobp.2020.04.013

Targeting MerTK Enhances Adaptive Immune Responses After Radiation Therapy

Garth W. Tormoen, Tiffany C. Blair, Shelly Bambina, Gwen Kramer, Jason Baird, Ramtin Rahmani, John M. Holland, Owen J.T. McCarty, Michael J. Baine, Vivek Verma, Nima Nabavizadeh, Michael J. Gough, Marka Crittenden

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21 Scopus citations

Abstract

Purpose: The role of MerTK, a member of the Tyro3-Axl-MerTK family of receptor tyrosine kinase, in the immune response to radiation therapy (RT) is unclear. We investigated immune-mediated tumor control after RT in murine models of colorectal and pancreatic adenocarcinoma using MerTK wild-type and knock-out hosts and whether inhibition of MerTK signaling with warfarin could replicate MerTK knock-out phenotypes. Methods and Materials: Wild-type and MerTK^–/– BALB/c mice were grafted in the flanks with CT26 tumors and treated with computed tomography guided RT. The role of macrophages and CD8 T cells in the response to radiation were demonstrated with cell depletion studies. The role of MerTK in priming immune responses after RT alone and with agonist antibodies to the T cell costimulatory molecule OX40 was evaluated in a Panc02-SIY model antigen system. The effect of warfarin therapy on the in-field and abscopal response to RT was demonstrated in murine models of colorectal adenocarcinoma. The association between warfarin and progression-free survival for patients treated with SABR for early-stage non-small cell lung cancer was evaluated in a multi-institutional retrospective study. Results: MerTK^–/– hosts had better tumor control after RT compared with wild-type mice in a macrophage and CD8 T cell–dependent manner. MerTK^–/– mice showed increased counts of tumor antigen-specific CD8 T cells in the peripheral blood after tumor-directed RT alone and in combination with agonist anti-OX40. Warfarin therapy phenocopied MerTK^–/– for single-flank tumors treated with RT and improved abscopal responses for RT combined with anti-CTLA4. Patients on warfarin therapy when treated with SABR for non-small cell lung cancer had higher progression-free survival rates compared with non–warfarin users. Conclusions: MerTK inhibits adaptive immune responses after SABR. Because warfarin inhibits MerTK signaling and phenocopies genetic deletion of MerTK in mice, warfarin therapy may have beneficial effects in combination with SABR and immune therapy in patients with cancer.

Original language	English (US)
Pages (from-to)	93-103
Number of pages	11
Journal	International Journal of Radiation Oncology Biology Physics
Volume	108
Issue number	1
DOIs	https://doi.org/10.1016/j.ijrobp.2020.04.013
State	Published - Sep 1 2020

ASJC Scopus subject areas

Radiation
Oncology
Radiology Nuclear Medicine and imaging
Cancer Research

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10.1016/j.ijrobp.2020.04.013

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Tormoen, G. W., Blair, T. C., Bambina, S., Kramer, G., Baird, J., Rahmani, R., Holland, J. M., McCarty, O. J. T., Baine, M. J., Verma, V., Nabavizadeh, N., Gough, M. J., & Crittenden, M. (2020). Targeting MerTK Enhances Adaptive Immune Responses After Radiation Therapy. International Journal of Radiation Oncology Biology Physics, 108(1), 93-103. https://doi.org/10.1016/j.ijrobp.2020.04.013

Tormoen, GW, Blair, TC, Bambina, S, Kramer, G, Baird, J, Rahmani, R, Holland, JM, McCarty, OJT, Baine, MJ, Verma, V, Nabavizadeh, N, Gough, MJ & Crittenden, M 2020, 'Targeting MerTK Enhances Adaptive Immune Responses After Radiation Therapy', International Journal of Radiation Oncology Biology Physics, vol. 108, no. 1, pp. 93-103. https://doi.org/10.1016/j.ijrobp.2020.04.013

@article{1f6bb28164894f93b7808755ab42e57c,

title = "Targeting MerTK Enhances Adaptive Immune Responses After Radiation Therapy",

abstract = "Purpose: The role of MerTK, a member of the Tyro3-Axl-MerTK family of receptor tyrosine kinase, in the immune response to radiation therapy (RT) is unclear. We investigated immune-mediated tumor control after RT in murine models of colorectal and pancreatic adenocarcinoma using MerTK wild-type and knock-out hosts and whether inhibition of MerTK signaling with warfarin could replicate MerTK knock-out phenotypes. Methods and Materials: Wild-type and MerTK–/– BALB/c mice were grafted in the flanks with CT26 tumors and treated with computed tomography guided RT. The role of macrophages and CD8 T cells in the response to radiation were demonstrated with cell depletion studies. The role of MerTK in priming immune responses after RT alone and with agonist antibodies to the T cell costimulatory molecule OX40 was evaluated in a Panc02-SIY model antigen system. The effect of warfarin therapy on the in-field and abscopal response to RT was demonstrated in murine models of colorectal adenocarcinoma. The association between warfarin and progression-free survival for patients treated with SABR for early-stage non-small cell lung cancer was evaluated in a multi-institutional retrospective study. Results: MerTK–/– hosts had better tumor control after RT compared with wild-type mice in a macrophage and CD8 T cell–dependent manner. MerTK–/– mice showed increased counts of tumor antigen-specific CD8 T cells in the peripheral blood after tumor-directed RT alone and in combination with agonist anti-OX40. Warfarin therapy phenocopied MerTK–/– for single-flank tumors treated with RT and improved abscopal responses for RT combined with anti-CTLA4. Patients on warfarin therapy when treated with SABR for non-small cell lung cancer had higher progression-free survival rates compared with non–warfarin users. Conclusions: MerTK inhibits adaptive immune responses after SABR. Because warfarin inhibits MerTK signaling and phenocopies genetic deletion of MerTK in mice, warfarin therapy may have beneficial effects in combination with SABR and immune therapy in patients with cancer.",

author = "Tormoen, {Garth W.} and Blair, {Tiffany C.} and Shelly Bambina and Gwen Kramer and Jason Baird and Ramtin Rahmani and Holland, {John M.} and McCarty, {Owen J.T.} and Baine, {Michael J.} and Vivek Verma and Nima Nabavizadeh and Gough, {Michael J.} and Marka Crittenden",

note = "Publisher Copyright: {\textcopyright} 2020 Elsevier Inc.",

year = "2020",

month = sep,

day = "1",

doi = "10.1016/j.ijrobp.2020.04.013",

language = "English (US)",

volume = "108",

pages = "93--103",

journal = "International Journal of Radiation Oncology Biology Physics",

issn = "0360-3016",

publisher = "Elsevier Inc.",

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T1 - Targeting MerTK Enhances Adaptive Immune Responses After Radiation Therapy

AU - Tormoen, Garth W.

AU - Blair, Tiffany C.

AU - Bambina, Shelly

AU - Kramer, Gwen

AU - Baird, Jason

AU - Rahmani, Ramtin

AU - Holland, John M.

AU - McCarty, Owen J.T.

AU - Baine, Michael J.

AU - Verma, Vivek

AU - Nabavizadeh, Nima

AU - Gough, Michael J.

AU - Crittenden, Marka

PY - 2020/9/1

Y1 - 2020/9/1

N2 - Purpose: The role of MerTK, a member of the Tyro3-Axl-MerTK family of receptor tyrosine kinase, in the immune response to radiation therapy (RT) is unclear. We investigated immune-mediated tumor control after RT in murine models of colorectal and pancreatic adenocarcinoma using MerTK wild-type and knock-out hosts and whether inhibition of MerTK signaling with warfarin could replicate MerTK knock-out phenotypes. Methods and Materials: Wild-type and MerTK–/– BALB/c mice were grafted in the flanks with CT26 tumors and treated with computed tomography guided RT. The role of macrophages and CD8 T cells in the response to radiation were demonstrated with cell depletion studies. The role of MerTK in priming immune responses after RT alone and with agonist antibodies to the T cell costimulatory molecule OX40 was evaluated in a Panc02-SIY model antigen system. The effect of warfarin therapy on the in-field and abscopal response to RT was demonstrated in murine models of colorectal adenocarcinoma. The association between warfarin and progression-free survival for patients treated with SABR for early-stage non-small cell lung cancer was evaluated in a multi-institutional retrospective study. Results: MerTK–/– hosts had better tumor control after RT compared with wild-type mice in a macrophage and CD8 T cell–dependent manner. MerTK–/– mice showed increased counts of tumor antigen-specific CD8 T cells in the peripheral blood after tumor-directed RT alone and in combination with agonist anti-OX40. Warfarin therapy phenocopied MerTK–/– for single-flank tumors treated with RT and improved abscopal responses for RT combined with anti-CTLA4. Patients on warfarin therapy when treated with SABR for non-small cell lung cancer had higher progression-free survival rates compared with non–warfarin users. Conclusions: MerTK inhibits adaptive immune responses after SABR. Because warfarin inhibits MerTK signaling and phenocopies genetic deletion of MerTK in mice, warfarin therapy may have beneficial effects in combination with SABR and immune therapy in patients with cancer.

AB - Purpose: The role of MerTK, a member of the Tyro3-Axl-MerTK family of receptor tyrosine kinase, in the immune response to radiation therapy (RT) is unclear. We investigated immune-mediated tumor control after RT in murine models of colorectal and pancreatic adenocarcinoma using MerTK wild-type and knock-out hosts and whether inhibition of MerTK signaling with warfarin could replicate MerTK knock-out phenotypes. Methods and Materials: Wild-type and MerTK–/– BALB/c mice were grafted in the flanks with CT26 tumors and treated with computed tomography guided RT. The role of macrophages and CD8 T cells in the response to radiation were demonstrated with cell depletion studies. The role of MerTK in priming immune responses after RT alone and with agonist antibodies to the T cell costimulatory molecule OX40 was evaluated in a Panc02-SIY model antigen system. The effect of warfarin therapy on the in-field and abscopal response to RT was demonstrated in murine models of colorectal adenocarcinoma. The association between warfarin and progression-free survival for patients treated with SABR for early-stage non-small cell lung cancer was evaluated in a multi-institutional retrospective study. Results: MerTK–/– hosts had better tumor control after RT compared with wild-type mice in a macrophage and CD8 T cell–dependent manner. MerTK–/– mice showed increased counts of tumor antigen-specific CD8 T cells in the peripheral blood after tumor-directed RT alone and in combination with agonist anti-OX40. Warfarin therapy phenocopied MerTK–/– for single-flank tumors treated with RT and improved abscopal responses for RT combined with anti-CTLA4. Patients on warfarin therapy when treated with SABR for non-small cell lung cancer had higher progression-free survival rates compared with non–warfarin users. Conclusions: MerTK inhibits adaptive immune responses after SABR. Because warfarin inhibits MerTK signaling and phenocopies genetic deletion of MerTK in mice, warfarin therapy may have beneficial effects in combination with SABR and immune therapy in patients with cancer.

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Targeting MerTK Enhances Adaptive Immune Responses After Radiation Therapy

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