NOX4 Inhibition Potentiates Immunotherapy by Overcoming Cancer-Associated Fibroblast-Mediated CD8 T-cell Exclusion from Tumors

Kirsty Ford(University of Southampton), Christopher J. Hanley(University of Southampton), Massimiliano Mellone(University of Southampton), Cédric Szyndralewiez(Genkyotex (Switzerland)), Freddy Heitz(Genkyotex (Switzerland)), Philippe Wiesel(Genkyotex (Switzerland)), Oliver Wood(University of Southampton), Maria do Céu Machado(University of Southampton), Maria‐Antoinette Lopez(University of Southampton), Anusha-Preethi Ganesan(La Jolla Institute for Immunology), Chuan Wang(University of Southampton), Ankur Chakravarthy(University of Toronto), Tim R. Fenton(University of Kent), Emma V. King(University of Southampton), Pandurangan Vijayanand(La Jolla Institute for Immunology), Christian H. Ottensmeier(University of Southampton), Aymen Al‐Shamkhani(University of Southampton), Natalia Savelyeva(University of Southampton), Gareth J. Thomas(University of Southampton)
Cancer Research
March 2, 2020
10.1158/0008-5472.can-19-3158
Cited by 427Open Access
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Abstract

Abstract Determining mechanisms of resistance to αPD-1/PD-L1 immune-checkpoint immunotherapy is key to developing new treatment strategies. Cancer-associated fibroblasts (CAF) have many tumor-promoting functions and promote immune evasion through multiple mechanisms, but as yet, no CAF-specific inhibitors are clinically available. Here we generated CAF-rich murine tumor models (TC1, MC38, and 4T1) to investigate how CAFs influence the immune microenvironment and affect response to different immunotherapy modalities [anticancer vaccination, TC1 (HPV E7 DNA vaccine), αPD-1, and MC38] and found that CAFs broadly suppressed response by specifically excluding CD8+ T cells from tumors (not CD4+ T cells or macrophages); CD8+ T-cell exclusion was similarly present in CAF-rich human tumors. RNA sequencing of CD8+ T cells from CAF-rich murine tumors and immunochemistry analysis of human tumors identified significant upregulation of CTLA-4 in the absence of other exhaustion markers; inhibiting CTLA-4 with a nondepleting antibody overcame the CD8+ T-cell exclusion effect without affecting Tregs. We then examined the potential for CAF targeting, focusing on the ROS-producing enzyme NOX4, which is upregulated by CAF in many human cancers, and compared this with TGFβ1 inhibition, a key regulator of the CAF phenotype. siRNA knockdown or pharmacologic inhibition [GKT137831 (Setanaxib)] of NOX4 “normalized” CAF to a quiescent phenotype and promoted intratumoral CD8+ T-cell infiltration, overcoming the exclusion effect; TGFβ1 inhibition could prevent, but not reverse, CAF differentiation. Finally, NOX4 inhibition restored immunotherapy response in CAF-rich tumors. These findings demonstrate that CAF-mediated immunotherapy resistance can be effectively overcome through NOX4 inhibition and could improve outcome in a broad range of cancers. Significance: NOX4 is critical for maintaining the immune-suppressive CAF phenotype in tumors. Pharmacologic inhibition of NOX4 potentiates immunotherapy by overcoming CAF-mediated CD8+ T-cell exclusion.

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