Literature DB >> 23545780

IFNβ/TNFα synergism induces a non-canonical STAT2/IRF9-dependent pathway triggering a novel DUOX2 NADPH oxidase-mediated airway antiviral response.

Karin Fink1, Lydie Martin, Esperance Mukawera, Stéfany Chartier, Xavier De Deken, Emmanuelle Brochiero, Françoise Miot, Nathalie Grandvaux.   

Abstract

Airway epithelial cells are key initial innate immune responders in the fight against respiratory viruses, primarily via the secretion of antiviral and proinflammatory cytokines that act in an autocrine/paracrine fashion to trigger the establishment of an antiviral state. It is currently thought that the early antiviral state in airway epithelial cells primarily relies on IFNβ secretion and the subsequent activation of the interferon-stimulated gene factor 3 (ISGF3) transcription factor complex, composed of STAT1, STAT2 and IRF9, which regulates the expression of a panoply of interferon-stimulated genes encoding proteins with antiviral activities. However, the specific pathways engaged by the synergistic action of different cytokines during viral infections, and the resulting physiological outcomes are still ill-defined. Here, we unveil a novel delayed antiviral response in the airways, which is initiated by the synergistic autocrine/paracrine action of IFNβ and TNFα, and signals through a non-canonical STAT2- and IRF9-dependent, but STAT1-independent cascade. This pathway ultimately leads to the late induction of the DUOX2 NADPH oxidase expression. Importantly, our study uncovers that the development of the antiviral state relies on DUOX2-dependent H2O2 production. Key antiviral pathways are often targeted by evasion strategies evolved by various pathogenic viruses. In this regard, the importance of the novel DUOX2-dependent antiviral pathway is further underlined by the observation that the human respiratory syncytial virus is able to subvert DUOX2 induction.

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Year:  2013        PMID: 23545780      PMCID: PMC3641604          DOI: 10.1038/cr.2013.47

Source DB:  PubMed          Journal:  Cell Res        ISSN: 1001-0602            Impact factor:   25.617


  56 in total

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3.  All-trans retinoic acid mediates DUOX2 expression and function in respiratory tract epithelium.

Authors:  Angela Lee Linderholm; June Onitsuka; Changhong Xu; Maggie Chiu; Wai-Ming Lee; Richart W Harper
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4.  Respiratory syncytial virus-mediated NF-kappa B p65 phosphorylation at serine 536 is dependent on RIG-I, TRAF6, and IKK beta.

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6.  Dual role of NOX2 in respiratory syncytial virus- and sendai virus-induced activation of NF-kappaB in airway epithelial cells.

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Review 7.  Mechanisms and function of DUOX in epithelia of the lung.

Authors:  Horst Fischer
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10.  Evaluation of the Calu-3 cell line as a model of in vitro respiratory syncytial virus infection.

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  32 in total

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Review 2.  Dual oxidase: a novel therapeutic target in allergic disease.

Authors:  Albert van der Vliet; Karamatullah Danyal; David E Heppner
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3.  VAMP8 Contributes to the TRIM6-Mediated Type I Interferon Antiviral Response during West Nile Virus Infection.

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4.  Noncanonical Effects of IRF9 in Intestinal Inflammation: More than Type I and Type III Interferons.

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Review 5.  Type I interferon in rheumatic diseases.

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6.  Airway epithelial dual oxidase 1 mediates allergen-induced IL-33 secretion and activation of type 2 immune responses.

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