ATM inhibition augments type I interferon response and antitumor T-cell immunity when combined with radiation therapy in murine tumor models

Won Jong Jin; Luke M Zangl; Meredith Hyun; Elian Massoud; Kaleb Schroeder; Roxana A Alexandridis; Zachary S Morris

doi:10.1136/jitc-2023-007474

ATM inhibition augments type I interferon response and antitumor T-cell immunity when combined with radiation therapy in murine tumor models

J Immunother Cancer. 2023 Sep;11(9):e007474. doi: 10.1136/jitc-2023-007474.

Authors

Won Jong Jin¹, Luke M Zangl¹, Meredith Hyun², Elian Massoud¹, Kaleb Schroeder¹, Roxana A Alexandridis², Zachary S Morris³

Affiliations

¹ Department Human Oncology, University of Wisconsin-Madison, Madison, Wisconsin, USA.
² Department of Biostatistics and Medical Informatics, University of Wisconsin-Madison, Madison, Wisconsin, USA.
³ Department Human Oncology, University of Wisconsin-Madison, Madison, Wisconsin, USA zmorris@humonc.wisc.edu.

Abstract

Background: Radiation therapy (RT) elicits DNA double-strand breaks, resulting in tumor cytotoxicity and a type I interferon (IFN) response via stimulator of interferon genes (STING) activation. We investigated whether combining RT with an ataxia-telangiectasia mutated inhibitor promoted these effects and amplified tumor immunity.

Methods: Mice-bearing syngeneic flank tumors (MOC2 head and neck squamous cell carcinoma or B78 melanoma) were treated with tumor-directed RT and oral administration of AZD0156. Specific immune cell depletion, type 1 interferon receptor 1 knock-out mice (IFNAR1-KO), and STING-deficient tumor cells were used to investigate tumor-immune crosstalk following RT and AZD0156 treatment.

Results: Combining RT and AZD0156 reduced tumor growth compared with RT or AZD0156 alone in mice bearing MOC2 or B78 tumors. Low-dose AZD0156 (1-100 nM) alone did not affect tumor cell proliferation but suppressed tumor cell clonogenicity in combination with RT. Low-dose AZD0156 with RT synergistically increased IFN-β, major histocompatibility complex (MHC)-I, and programmed death-ligand 1 (PD-L1) expression in tumor cells. In contrast to wild-type mice, IFNAR1-KO mice showed reduced CD8+T cell tumor infiltration and poor survival following RT+AZD0156 treatment. CD8+T cell depletion reduced antitumor response during RT+AZD0156 treatment. STING-deficient MOC2 (MOC2-STING+/-) or B78 (B78-STING-/-) tumors eliminated the effects of RT+AZD0156 on the expression of IFN-β, MHC-I, and PD-L1, and reduced CD8+T cell infiltration and migration. Additional anti-PD-L1 therapy promoted antitumor response by elevation of tumor-MHC-I and lymphocyte activation.

Conclusions: Combined radiation and AZD0156 increase STING-dependent antitumor response. Tumor-derived cell-autonomous IFN-β amplification drives both MHC-I and PD-L1 induction at the tumor cell surface, which is required by anti-PD-L1 therapy to promote antitumor immune response following RT and AZD0156 combination therapy.

Keywords: Adaptive Immunity; Drug Evaluation, Preclinical; Drug Therapy, Combination; Immune Checkpoint Inhibitors; RADIOTHERAPY.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Administration, Oral
Animals
CD8-Positive T-Lymphocytes*
Cell Membrane
Combined Modality Therapy
Melanoma*
Mice

Abstract

Publication types

MeSH terms

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