Abstract

Ebola viruses (EBOVs) are NIAID category A priority pathogens that cause severe viral hemorrhagic fever. A critical research task is to define how the molecular interactions between filoviruses and the human host trigger life-threatening infections. Defining such interactions will shed light on the triggers of viral hemorrhagic fever and will facilitate prophylactic and therapeutic interventions for this frequently lethal syndrome. We hypothesize that evasion of host innate defenses, particularly interferon (IFN)-??? responses, is critical to the uncontrolled virus replication and inflammation characteristic of EBOV infections. We previously demonstrated that the EBOV VP35 protein inhibits production of IFN??? and, consistent with a critical role for VP35 as a virulence factor, a VP35 mutant EBOV defective for suppression of IFN??? responses was avirulent in guinea pigs. We also demonstrated that that the EBOV VP24 protein inhibits IFN-induced Jak-STAT signaling by preventing the trafficking of phosphorylated STAT1 to the nucleus. This project builds upon these and other observations regarding the function of VP35 and VP24 to define their mechanisms of action, their impact on EBOV replication and their impact on EBOV pathogenesis. Based on data demonstrating that interaction of VP24 with karyopherin alpha nuclear localization signal receptors inhibits phospho-STAT1 nuclear import, we will define the mechanism by which VP24 blocks STAT1 nuclear import and assess the impact of VP24 on the nucleo/cytoplasmic trafficking of other karyopherin alpha cargoes. We also observed that VP24 inhibits the induction of cellular antioxidant responses normally mediated by the transcription factor Nrf2. Because Nrf2- induced antioxidant responses have been increasingly implicated in responses, including innate immune responses, to virus infection;we will determine the mechanism by which EBOV VP24 inhibits the Nrf2-induced antioxidant responses and the consequences of this inhibition for innate immunity. As multiple mechanisms have been identified by which EBOV VP35 inhibits IFN??? signaling, including sequestration of dsRNAs, interference with the kinases IKK? and TBK-1 and inhibition of interferon regulatory factor 7 function;we will dissect out the contribution of these functions to inhibition of IFN??? production. Finally, mutant recombinant EBOVs will be generated to determine how VP24 and VP35 immune evasion functions contribute to viral replication and virulence. The results of these studies will shed light on the contribution of VP24 and VP35 to EBOV pathogenesis and identify viral functions that may be targeted for antiviral development.

Public Health Relevance

Ebolaviruses (EBOVs) are emerging viruses that cause severe viral hemorrhagic fevers and are therefore considered a public health threat. Currently, the factors used by these viruses to cause severe illness are not well-defined. The experiments in this proposal will clarify the role of two viral proteins, VP24 and VP35, in EBOV disease and suggest new ways to prevent or treat these infections.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI059536-07
Application #
8204787
Study Section
Virology - B Study Section (VIRB)
Program Officer
Repik, Patricia M
Project Start
2004-04-01
Project End
2015-11-30
Budget Start
2011-12-01
Budget End
2012-11-30
Support Year
7
Fiscal Year
2012
Total Cost
$437,614
Indirect Cost
$106,047

  Institution

Name
Icahn School of Medicine at Mount Sinai
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
078861598
City
New York
State
NY
Country
United States
Zip Code
10029

  Publications

Yen, Benjamin C; Basler, Christopher F (2016) Effects of Filovirus Interferon Antagonists on Responses of Human Monocyte-Derived Dendritic Cells to RNA Virus Infection. J Virol 90:5108-5118
Edwards, Megan R; Liu, Gai; Mire, Chad E et al. (2016) Differential Regulation of Interferon Responses by Ebola and Marburg Virus VP35 Proteins. Cell Rep 14:1632-1640
Basler, Christopher F (2015) Innate immune evasion by filoviruses. Virology 479-480:122-30
Luthra, Priya; Jordan, David S; Leung, Daisy W et al. (2015) Ebola virus VP35 interaction with dynein LC8 regulates viral RNA synthesis. J Virol 89:5148-53
Messaoudi, Ilhem; Basler, Christopher F (2015) Immunological features underlying viral hemorrhagic fevers. Curr Opin Immunol 36:38-46
Messaoudi, Ilhem; Amarasinghe, Gaya K; Basler, Christopher F (2015) Filovirus pathogenesis and immune evasion: insights from Ebola virus and Marburg virus. Nat Rev Microbiol 13:663-76
Feagins, Alicia R; Basler, Christopher F (2015) Amino Acid Residue at Position 79 of Marburg Virus VP40 Confers Interferon Antagonism in Mouse Cells. J Infect Dis 212 Suppl 2:S219-25
Edwards, Megan R; Basler, Christopher F (2015) Marburg Virus VP24 Protein Relieves Suppression of the NF-?B Pathway Through Interaction With Kelch-like ECH-Associated Protein 1. J Infect Dis 212 Suppl 2:S154-9
Leung, Daisy W; Borek, Dominika; Luthra, Priya et al. (2015) An Intrinsically Disordered Peptide from Ebola Virus VP35 Controls Viral RNA Synthesis by Modulating Nucleoprotein-RNA Interactions. Cell Rep 11:376-89
Teixeira, Avelino; Yen, Benjamin; Gusella, Gabriele Luca et al. (2015) Prothymosin ? variants isolated from CD8+ T cells and cervicovaginal fluid suppress HIV-1 replication through type I interferon induction. J Infect Dis 211:1467-75

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