Tumor-intrinsic IRE1α signaling controls protective immunity in lung cancer

Author:

Crowley Michael J. P.,Bhinder Bhavneet,Markowitz Geoffrey J.ORCID,Martin Mitchell,Verma Akanksha,Sandoval Tito A.ORCID,Chae Chang-Suk,Yomtoubian Shira,Hu YangORCID,Chopra SahilORCID,Tavarez Diamile A.,Giovanelli PaoloORCID,Gao DingchengORCID,McGraw Timothy E.ORCID,Altorki Nasser K.ORCID,Elemento OlivierORCID,Cubillos-Ruiz Juan R.ORCID,Mittal VivekORCID

Abstract

AbstractIRE1α-XBP1 signaling is emerging as a central orchestrator of malignant progression and immunosuppression in various cancer types. Employing a computational XBP1s detection method applied to TCGA datasets, we demonstrate that expression of the XBP1s mRNA isoform predicts poor survival in non-small cell lung cancer (NSCLC) patients. Ablation of IRE1α in malignant cells delays tumor progression and extends survival in mouse models of NSCLC. This protective effect is accompanied by alterations in intratumoral immune cell subsets eliciting durable adaptive anti-cancer immunity. Mechanistically, cancer cell-intrinsic IRE1α activation sustains mPGES-1 expression, enabling production of the immunosuppressive lipid mediator prostaglandin E2. Accordingly, restoring mPGES-1 expression in IRE1αKO cancer cells rescues normal tumor progression. We have developed an IRE1α gene signature that predicts immune cell infiltration and overall survival in human NSCLC. Our study unveils an immunoregulatory role for cancer cell-intrinsic IRE1α activation and suggests that targeting this pathway may help enhance anti-tumor immunity in NSCLC.

Funder

U.S. Department of Health & Human Services | National Institutes of Health

United States Department of Defense | United States Army | Army Medical Command | Congressionally Directed Medical Research Programs

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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