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. 2019 Jan;25(1):95-102.
doi: 10.1038/s41591-018-0302-5. Epub 2018 Dec 17.

Tumor-derived IFN triggers chronic pathway agonism and sensitivity to ADAR loss

Huayang Liu  1 Javad Golji  1 Lauren K Brodeur  1 Franklin S Chung  1 Julie T Chen  1 Rosalie S deBeaumont  1 Caroline P Bullock  1 Michael D Jones  1 Grainne Kerr  2 Li Li  1 Daniel P Rakiec  1 Michael R Schlabach  1 Sosathya Sovath  1 Joseph D Growney  1 Raymond A Pagliarini  1 David A Ruddy  1 Kenzie D MacIsaac  1 Joshua M Korn  1 E Robert McDonald 3rd  3
Affiliations

Tumor-derived IFN triggers chronic pathway agonism and sensitivity to ADAR loss

Huayang Liu et al. Nat Med. 2019 Jan.

Abstract

Interferons (IFNs) are cytokines that play a critical role in limiting infectious and malignant diseases 1-4 . Emerging data suggest that the strength and duration of IFN signaling can differentially impact cancer therapies, including immune checkpoint blockade 5-7 . Here, we characterize the output of IFN signaling, specifically IFN-stimulated gene (ISG) signatures, in primary tumors from The Cancer Genome Atlas. While immune infiltration correlates with the ISG signature in some primary tumors, the existence of ISG signature-positive tumors without evident infiltration of IFN-producing immune cells suggests that cancer cells per se can be a source of IFN production. Consistent with this hypothesis, analysis of patient-derived tumor xenografts propagated in immune-deficient mice shows evidence of ISG-positive tumors that correlates with expression of human type I and III IFNs derived from the cancer cells. Mechanistic studies using cell line models from the Cancer Cell Line Encyclopedia that harbor ISG signatures demonstrate that this is a by-product of a STING-dependent pathway resulting in chronic tumor-derived IFN production. This imposes a transcriptional state on the tumor, poising it to respond to the aberrant accumulation of double-stranded RNA (dsRNA) due to increased sensor levels (MDA5, RIG-I and PKR). By interrogating our functional short-hairpin RNA screen dataset across 398 cancer cell lines, we show that this ISG transcriptional state creates a novel genetic vulnerability. ISG signature-positive cancer cells are sensitive to the loss of ADAR, a dsRNA-editing enzyme that is also an ISG. A genome-wide CRISPR genetic suppressor screen reveals that the entire type I IFN pathway and the dsRNA-activated kinase, PKR, are required for the lethality induced by ADAR depletion. Therefore, tumor-derived IFN resulting in chronic signaling creates a cellular state primed to respond to dsRNA accumulation, rendering ISG-positive tumors susceptible to ADAR loss.

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