Sensitizing immune unresponsive colorectal cancers to immune checkpoint inhibitors through MAVS overexpression

Bin-Jin Hwang; Li-Chung Tsao; Chaitanya R Acharya; Timothy Trotter; Pankaj Agarwal; Junping Wei; Tao Wang; Xiao-Yi Yang; Gangjun Lei; Takuya Osada; Herbert Kim Lyerly; Michael A Morse; Zachary Conrad Hartman

doi:10.1136/jitc-2021-003721

Sensitizing immune unresponsive colorectal cancers to immune checkpoint inhibitors through MAVS overexpression

J Immunother Cancer. 2022 Mar;10(3):e003721. doi: 10.1136/jitc-2021-003721.

Authors

Bin-Jin Hwang¹, Li-Chung Tsao¹, Chaitanya R Acharya¹, Timothy Trotter¹, Pankaj Agarwal¹, Junping Wei¹, Tao Wang¹, Xiao-Yi Yang¹, Gangjun Lei¹, Takuya Osada¹, Herbert Kim Lyerly^{1

2

3}, Michael A Morse^{1

4}, Zachary Conrad Hartman^{5

3}

Affiliations

¹ Surgery, Duke University, Durham, North Carolina, USA.
² Immunology, Duke University, Durham, North Carolina, USA.
³ Pathology, Duke University, Durham, North Carolina, USA.
⁴ Medicine, Duke University, Durham, NC, USA.
⁵ Surgery, Duke University, Durham, North Carolina, USA zachary.hartman@duke.edu.

Abstract

Background: The majority of colorectal carcinomas (CRCs) are insensitive to programmed death protein-1/programmed death-ligand 1 (anti-PD-1/PD-L1) immune checkpoint inhibitor (ICI) antibodies. While there are many causes for ICI insensitivity, recent studies suggest that suppression of innate immune gene expression in tumor cells could be a root cause of this insensitivity and an important factor in the evolution of tumor immunosuppression.

Methods: We first assessed the reduction of mitochondrial antiviral signaling gene (MAVS) and related RIG-I pathway gene expression in several patient RNA expression datasets. We then engineered MAVS expressing tumor cells and tested their ability to elicit innate and adaptive anti-tumor immunity using both in vitro and in vivo approaches, which we then confirmed using MAVS expressing viral vectors. Finally, we observed that MAVS stimulated PD-L1 expression in multiple cell types and then assessed the combination of PD-L1 ICI antibodies with MAVS tumor expression in vivo.

Results: MAVS was significantly downregulated in CRCs, but its re-expression could stimulate broad cellular interferon-related responses, in both murine and patient-derived CRCs. In vivo, local MAVS expression elicited significant anti-tumor responses in both immune-sensitive and insensitive CRC models, through the stimulation of an interferon responsive axis that provoked tumor antigen-specific adaptive immunity. Critically, we found that tumor-intrinsic MAVS expression triggered systemic adaptive immune responses that enabled abscopal CD8 +T cell cytotoxicity against distant CRCs. As MAVS also induced PD-L1 expression, we further found synergistic anti-tumor responses in combination with anti-PD-L1 ICIs.

Conclusion: These data demonstrate that intratumoral MAVS expression results in local and systemic tumor antigen-specific T cell responses, which could be combined with PD-L1 ICI to permit effective anti-tumor immunotherapy in ICI resistant cancers.

Keywords: immunity, innate; immunotherapy.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Animals
Antiviral Agents
Colorectal Neoplasms* / drug therapy
Colorectal Neoplasms* / genetics
Humans
Immune Checkpoint Inhibitors* / pharmacology
Immune Checkpoint Inhibitors* / therapeutic use
Immunotherapy / methods
Mice
Signal Transduction

Substances

Antiviral Agents
Immune Checkpoint Inhibitors

Abstract

Publication types

MeSH terms

Substances

Grants and funding