Abstract

Systematic exploration of cancer cell vulnerabilities can inform the development of novel cancer therapeutics. Here, through analysis of genome-scale loss-of-function datasets, we identify adenosine deaminase acting on RNA (ADAR or ADAR1) as an essential gene for the survival of a subset of cancer cell lines. ADAR1-dependent cell lines display increased expression of interferon-stimulated genes. Activation of type I interferon signaling in the context of ADAR1 deficiency can induce cell lethality in non-ADAR1-dependent cell lines. ADAR deletion causes activation of the double-stranded RNA sensor, protein kinase R (PKR). Disruption of PKR signaling, through inactivation of PKR or overexpression of either a wildtype or catalytically inactive mutant version of the p150 isoform of ADAR1, partially rescues cell lethality after ADAR1 loss, suggesting that both catalytic and non-enzymatic functions of ADAR1 may contribute to preventing PKR-mediated cell lethality. Together, these data nominate ADAR1 as a potential therapeutic target in a subset of cancers.

Specific cancer cell vulnerabilities can provide an opportunity for the development of novel cancer therapeutics. In this study the authors demonstrate that targeting ADAR1 represents a potential therapeutic vulnerability in cancers with activated interferon response signatures.

Details

Title
Identification of ADAR1 adenosine deaminase dependency in a subset of cancer cells
Author
Gannon, Hugh S 1 ; Zou Tao 1 ; Kiessling, Michael K 2 ; Gao, Galen F 3   VIAFID ORCID Logo  ; Cai, Diana 1 ; Choi, Peter S 1 ; Ivan, Alexandru P 4   VIAFID ORCID Logo  ; Buchumenski Ilana 5 ; Berger, Ashton C 3 ; Goldstein, Jonathan T 3 ; Cherniack, Andrew D 1   VIAFID ORCID Logo  ; Vazquez Francisca 3   VIAFID ORCID Logo  ; Tsherniak Aviad 3   VIAFID ORCID Logo  ; Levanon, Erez Y 5   VIAFID ORCID Logo  ; Hahn, William C 6   VIAFID ORCID Logo  ; Meyerson, Matthew 7   VIAFID ORCID Logo 

 Dana-Farber Cancer Institute, Department of Medical Oncology, Boston, USA (GRID:grid.65499.37) (ISNI:0000 0001 2106 9910); Broad Institute of Harvard and MIT, Cambridge, USA (GRID:grid.66859.34) (ISNI:0000 0004 0546 1623) 
 University of Zurich and University Hospital Zürich, Department of Gastroenterology and Hepatology, Zürich, Switzerland (GRID:grid.7400.3) (ISNI:0000 0004 1937 0650); University Hospital Zurich, University of Zurich, Department of Medical Oncology and Hematology, Zurich, Switzerland (GRID:grid.412004.3) (ISNI:0000 0004 0478 9977) 
 Broad Institute of Harvard and MIT, Cambridge, USA (GRID:grid.66859.34) (ISNI:0000 0004 0546 1623) 
 Dana-Farber Cancer Institute, Department of Medical Oncology, Boston, USA (GRID:grid.65499.37) (ISNI:0000 0001 2106 9910) 
 Bar-Ilan University, The Mina and Everard Goodman Faculty of Life Sciences, Ramat Gan, Israel (GRID:grid.22098.31) (ISNI:0000 0004 1937 0503) 
 Dana-Farber Cancer Institute, Department of Medical Oncology, Boston, USA (GRID:grid.65499.37) (ISNI:0000 0001 2106 9910); Broad Institute of Harvard and MIT, Cambridge, USA (GRID:grid.66859.34) (ISNI:0000 0004 0546 1623); Harvard Medical School, Department of Medicine, Brigham and Women’s Hospital, Boston, USA (GRID:grid.38142.3c) (ISNI:000000041936754X); Dana-Farber Cancer Institute, Center for Cancer Genome Discovery, Boston, USA (GRID:grid.65499.37) (ISNI:0000 0001 2106 9910) 
 Dana-Farber Cancer Institute, Department of Medical Oncology, Boston, USA (GRID:grid.65499.37) (ISNI:0000 0001 2106 9910); Broad Institute of Harvard and MIT, Cambridge, USA (GRID:grid.66859.34) (ISNI:0000 0004 0546 1623); Dana-Farber Cancer Institute, Center for Cancer Genome Discovery, Boston, USA (GRID:grid.65499.37) (ISNI:0000 0001 2106 9910); Harvard Medical School, Department of Pathology, Boston, USA (GRID:grid.38142.3c) (ISNI:000000041936754X) 
Publication year
2018
Publication date
2018
Publisher
Nature Publishing Group
e-ISSN
20411723
Source type
Scholarly Journal
Language of publication
English
DOI
https://doi.org/10.1038/s41467-018-07824-4
ProQuest document ID
2646021189
Copyright
© The Author(s) 2018. This work is published under http://creativecommons.org/licenses/by/4.0/ (the “License”). Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.