1. Suppression of type I interferon production by porcine epidemic diarrhea virus and degradation of CREB-binding protein by nsp1
- Author
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Dongwan Yoo, Kaichuang Shi, and Qingzhan Zhang
- Subjects
0301 basic medicine ,Swine ,viruses ,Down-Regulation ,Viral Nonstructural Proteins ,CBP ,medicine.disease_cause ,Article ,Enhanceosome ,03 medical and health sciences ,Virology ,medicine ,Animals ,Nsp1 ,Innate immune signaling ,CREB-binding protein ,Promoter Regions, Genetic ,Coronavirus ,Cell Nucleus ,Swine Diseases ,NSP1 ,Innate immune system ,biology ,Porcine epidemic diarrhea virus ,virus diseases ,Interferon regulation ,Interferon-beta ,biology.organism_classification ,Type I interferon production ,030104 developmental biology ,Host-Pathogen Interactions ,Proteolysis ,biology.protein ,Coronavirus Infections ,IRF3 ,Protein Binding - Abstract
Type I interferons (IFN-α/β) are the major components of the innate immune response of hosts, and in turn many viruses have evolved to modulate the host response during infection. We found that the IFN-β production was significantly suppressed during PEDV infection in cells. To identify viral IFN antagonists and to study their suppressive function, viral coding sequences for the entire structural and nonstructural proteins were cloned and expressed. Of 16 PEDV nonstructural proteins (nsps), nsp1, nsp3, nsp7, nsp14, nsp15 and nsp16 were found to inhibit the IFN-β and IRF3 promoter activities. The sole accessory protein ORF3, structure protein envelope (E), membrane (M), and nucleocapsid (N) protein were also shown to inhibit such activities. PEDV nsp1 did not interfere the IRF3 phosphorylation and nuclear translocation but interrupted the enhanceosome assembly of IRF3 and CREB-binding protein (CBP) by degrading CBP. A further study showed that the CBP degradation by nsp1 was proteasome-dependent. Our data demonstrate that PEDV modulates the host innate immune responses by degrading CBP and suppressing ISGs expression., Highlights • PEDV modulates the host innate immune system by suppressing the type I interferon production and ISGs expression. • Ten viral proteins were identified as IFN antagonists, and nsp1 was the most potent viral IFN antagonist. • PEDV nsp1 did not interfere the IRF3 phosphorylation and nuclear translocation but interrupted the enhanceosome assembly of IRF3 and CREB-binding protein (CBP). • PEDV nsp1 caused the CBP degradation in the nucleus, which may be the key mechanism for PEDV-mediated IFN downregulation.
- Published
- 2016
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