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Targeting innate immunity for antiviral therapy through small molecule agonists of the RLR pathway

Sowmya Pattabhi, Courtney R. Wilkins, Ran Dong, Megan L. Knoll, Jeffrey Posakony, Shari Kaiser, Chad E. Mire, Myra L. Wang, Renee C. Ireton, Thomas W. Geisbert, Kristin M. Bedard, Shawn P. Iadonato, Yueh-Ming Loo, Michael Gale Jr.
Sowmya Pattabhi
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
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Courtney R. Wilkins
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
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Ran Dong
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
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Megan L. Knoll
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
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Jeffrey Posakony
4KINETA Inc., Seattle, Washington, USA
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Shari Kaiser
4KINETA Inc., Seattle, Washington, USA
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Chad E. Mire
5University of Texas Medical Branch at Galveston, Galveston National Laboratory, Galveston, Texas, USA
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Myra L. Wang
4KINETA Inc., Seattle, Washington, USA
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Renee C. Ireton
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
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Thomas W. Geisbert
5University of Texas Medical Branch at Galveston, Galveston National Laboratory, Galveston, Texas, USA
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Kristin M. Bedard
4KINETA Inc., Seattle, Washington, USA
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Shawn P. Iadonato
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
4KINETA Inc., Seattle, Washington, USA
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Yueh-Ming Loo
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
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  • ORCID record for Yueh-Ming Loo
  • For correspondence: mgale@uw.edu looy@uw.edu
Michael Gale Jr.
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
1Departments of Global Health and 2 and Immunology 3the Center for Innate Immunity and Immune Disease, University of Washington, Seattle, Washington, USA
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  • For correspondence: mgale@uw.edu looy@uw.edu
DOI: 10.1128/JVI.02202-15
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ABSTRACT

The cellular response to virus infection is initiated when pathogen recognition receptors (PRR) engage viral pathogen associated molecular patterns (PAMPs). This process results in induction of downstream signaling pathways that activate the transcription factor IRF3. IRF3 plays a critical role in antiviral immunity to drive the expression of innate immune response genes, including those encoding antiviral factors, type 1 interferon, and immune modulatory cytokines that act in concert to restrict virus replication. Thus, small molecule agonists that can promote IRF3 activation and induce innate immune gene expression could serve as antivirals to induce tissue-wide innate immunity for effective control of virus infection. We identified small molecule compounds that activate IRF3 to differentially induce discrete subsets of antiviral genes. We tested a lead compound and derivatives for the ability to suppress infection by a broad range of RNA viruses. Compound administration significantly decreased the viral RNA load in cultured cells that were infected with the family Flaviviridae, including West Nile virus, dengue virus and hepatitis C virus as well as viruses of the families Filoviridae (Ebola virus), Orthomyxoviridae (influenza A virus), Arenaviridae (Lassa virus) and Paramyxoviridae (respiratory syncytial virus, Nipah virus) to suppress infectious virus production. Knockdown studies mapped this response to the RIG-I-like receptor pathway. This work identifies a novel class of host-directed immune modulatory molecules that activate IRF3 to promote host antiviral responses to broadly suppress infection by RNA viruses of distinct genera.

IMPORTANCE Incidences of emerging and re-emerging RNA viruses highlight a desperate need for broad-spectrum antiviral agents that can effectively control infection by viruses of distinct genera. We identified small molecule compounds that can selectively activate IRF3 for the purpose of identifying drug-like molecules that can be developed for the treatment of viral infections. Here, we report the discovery of a hydroxyquinoline family of small molecules that can activate IRF3 to promote cellular antiviral responses. These molecules can prophylactically or therapeutically control infection in cell culture by pathogenic RNA viruses including West Nile virus, dengue virus, hepatitis C virus, influenza A virus, respiratory syncytial virus, Nipah virus, Lassa virus and Ebola virus. Our study thus identifies a class of small molecules with novel mechanism to enhance host immune responses for antiviral activity against a variety of RNA viruses that pose a significant healthcare burden and/or with known high case fatality rates.

FOOTNOTES

  • ↵#Address correspondence to Michael Gale Jr., mgale{at}uw.edu and Yueh-Ming Loo, looy{at}uw.edu
  • Copyright © 2015, American Society for Microbiology. All Rights Reserved.
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Targeting innate immunity for antiviral therapy through small molecule agonists of the RLR pathway
Sowmya Pattabhi, Courtney R. Wilkins, Ran Dong, Megan L. Knoll, Jeffrey Posakony, Shari Kaiser, Chad E. Mire, Myra L. Wang, Renee C. Ireton, Thomas W. Geisbert, Kristin M. Bedard, Shawn P. Iadonato, Yueh-Ming Loo, Michael Gale Jr.
Journal of Virology Dec 2015, JVI.02202-15; DOI: 10.1128/JVI.02202-15

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Targeting innate immunity for antiviral therapy through small molecule agonists of the RLR pathway
Sowmya Pattabhi, Courtney R. Wilkins, Ran Dong, Megan L. Knoll, Jeffrey Posakony, Shari Kaiser, Chad E. Mire, Myra L. Wang, Renee C. Ireton, Thomas W. Geisbert, Kristin M. Bedard, Shawn P. Iadonato, Yueh-Ming Loo, Michael Gale Jr.
Journal of Virology Dec 2015, JVI.02202-15; DOI: 10.1128/JVI.02202-15
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