The Adenovirus E4orf4 Protein Provides a Novel Mechanism for Inhibition of the DNA Damage Response

Anna Brestovitsky; Keren Nebenzahl-Sharon; Peter Kechker; Rakefet Sharf; Tamar Kleinberger

doi:10.1371/journal.ppat.1005420

The Adenovirus E4orf4 Protein Provides a Novel Mechanism for Inhibition of the DNA Damage Response

PLoS Pathog. 2016 Feb 11;12(2):e1005420. doi: 10.1371/journal.ppat.1005420. eCollection 2016 Feb.

Authors

Anna Brestovitsky¹, Keren Nebenzahl-Sharon¹, Peter Kechker¹, Rakefet Sharf¹, Tamar Kleinberger¹

Affiliation

¹ Department of Microbiology, the Rappaport Faculty of Medicine and Research Institute, Technion-Israel Institute of Technology, Haifa, Israel.

Abstract

The DNA damage response (DDR) is a conglomerate of pathways designed to detect DNA damage and signal its presence to cell cycle checkpoints and to the repair machinery, allowing the cell to pause and mend the damage, or if the damage is too severe, to trigger apoptosis or senescence. Various DDR branches are regulated by kinases of the phosphatidylinositol 3-kinase-like protein kinase family, including ataxia-telangiectasia mutated (ATM) and ATM- and Rad3-related (ATR). Replication intermediates and linear double-stranded genomes of DNA viruses are perceived by the cell as DNA damage and activate the DDR. If allowed to operate, the DDR will stimulate ligation of viral genomes and will inhibit virus replication. To prevent this outcome, many DNA viruses evolved ways to limit the DDR. As part of its attack on the DDR, adenovirus utilizes various viral proteins to cause degradation of DDR proteins and to sequester the MRN damage sensor outside virus replication centers. Here we show that adenovirus evolved yet another novel mechanism to inhibit the DDR. The E4orf4 protein, together with its cellular partner PP2A, reduces phosphorylation of ATM and ATR substrates in virus-infected cells and in cells treated with DNA damaging drugs, and causes accumulation of damaged DNA in the drug-treated cells. ATM and ATR are not mutually required for inhibition of their signaling pathways by E4orf4. ATM and ATR deficiency as well as E4orf4 expression enhance infection efficiency. Furthermore, E4orf4, previously reported to induce cancer-specific cell death when expressed alone, sensitizes cells to killing by sub-lethal concentrations of DNA damaging drugs, likely because it inhibits DNA damage repair. These findings provide one explanation for the cancer-specificity of E4orf4-induced cell death as many cancers have DDR deficiencies leading to increased reliance on the remaining intact DDR pathways and to enhanced susceptibility to DDR inhibitors such as E4orf4. Thus DDR inhibition by E4orf4 contributes both to the efficiency of adenovirus replication and to the ability of E4orf4 to kill cancer cells.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adenoviridae Infections / virology*
Adenoviruses, Human / genetics
Adenoviruses, Human / physiology*
Ataxia Telangiectasia Mutated Proteins / genetics
Ataxia Telangiectasia Mutated Proteins / metabolism*
Cell Death
Cell Line, Tumor
DNA Damage*
DNA Repair
DNA Replication
Humans
Mutation
Phosphorylation
Signal Transduction
Viral Proteins / genetics
Viral Proteins / metabolism*
Virus Replication

Substances

E4orf4 protein, adenovirus
Viral Proteins
ATM protein, human
ATR protein, human
Ataxia Telangiectasia Mutated Proteins

Grants and funding

This work was supported by the Binational Science Foundation US-Israel, grant number 2013140 to TK, http://www.bsf.org.il; the Israel Cancer Association grant number 20150008 to TK, with the generous assistance of the ICA Switzerland friends, http://en.cancer.org.il/template_e/default.aspx?PageId=7606; and the Israel Science Foundation grant number 399/11 to TK, http://www.isf.org.il/english/default.asp. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.