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Proc Natl Acad Sci USA. Lessons learned and concepts formed from study of the pathogenesis of the two negative-strand viruses lymphocytic choriomeningitis and influenza

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  • Proc Natl Acad Sci USA. Lessons learned and concepts formed from study of the pathogenesis of the two negative-strand viruses lymphocytic choriomeningitis and influenza

    [Source: Proceedings of the National Academy of Sciences of the United States of America, full page: (LINK). Abstract, edited.]
    Lessons learned and concepts formed from study of the pathogenesis of the two negative-strand viruses lymphocytic choriomeningitis and influenza


    Michael B. A. Oldstone<SUP>1</SUP>
    <SUP></SUP>
    Author Affiliations: Viral Immunobiology Laboratory, Department of Immunology and Microbial Science, The Scripps Research Institute, La Jolla, CA 92037

    Contributed by Michael B. A. Oldstone, December 20, 2012 (sent for review December 5, 2012)



    Abstract

    Viruses have unique lifestyles. To describe the pathogenesis and significance of viral infection in terms of host responses, resultant injury, and therapy, we focused on two RNA viruses: lymphocytic choriomeningitis (LCMV) and influenza (Flu). Many of the currently established concepts and consequences about viruses and immunologic tolerance, virus-induced immunosuppression, virus-induced autoimmunity, immune complex disease, and virus?lymphocyte and virus?dendritic cell interactions evolved through studies of LCMV in its natural murine host. Similarly, the mechanisms, aftermath, and treatment of persistent RNA viruses emerged, in large part, from research on LCMV. Analysis of acute influenza virus infections uncovered the prominent direct role that cytokine storm plays in the pathogenesis, morbidity, and mortality from this disease. Cytokine storm of influenza virus infection is initiated via a pulmonary endothelial cell amplification loop involving IFN-producing cells and virus-infected pulmonary epithelial cells. Importantly, the cytokine storm is chemically treatable with specific agonist therapy directed to the sphingosphine 1 phosphate receptor 1, which is located on pulmonary endothelial cells, pointing to the endothelial cells as the gatekeepers of this hyperaggressive host immune response.

    viral persistence ? immunosupression



    Footnotes

    <SUP>1</SUP>E-mail: mbaobo@scripps.edu.

    This contribution is part of the special series of Inaugural Articles by members of the National Academy of Sciences elected in 2008.

    Author contributions: M.B.A.O. designed research, performed research for several experiments discussed, contributed new reagents/analytic tools, analyzed data, and wrote the paper.

    The author declares no conflict of interest.
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