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Herpes Simplex Virus Type 2 Inhibits Type I IFN Signaling Mediated by the Novel E3 Ubiquitin Protein Ligase Activity of Viral Protein ICP22

J Immunol. 2020-07-01; 
Mudan Zhang, Ming Fu, Miaomiao Li, Huimin Hu, Sitang Gong, Qinxue Hu
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Peptide Synthesis … 1 3 105 U/ml IFN-b for 16 h. Cells were lysed with WB/IP lysis buffer (P0013; Beyotime Biotechnology) containing protease … PurKine Anti-DYKDDDDK Tag Resin 4FF (BMR21504; Abbkine Scientific) and eluted with 250 mg/ml DYKDDDDK peptide (RP10586; GenScript, Nanj … Get A Quote

摘要

Type I IFNs play an important role in innate immunity against viral infections by inducing the expression of IFN-stimulated genes (ISGs), which encode effectors with various antiviral functions. We and others previously reported that HSV type 2 (HSV-2) inhibits the synthesis of type I IFNs, but how HSV-2 suppresses IFN-mediated signaling is less understood. In the current study, after the demonstration of HSV-2 replication resistance to IFN-β treatment in human epithelial cells, we reveal that HSV-2 and the viral protein ICP22 significantly decrease the expression of ISG54 at both mRNA and protein levels. Likewise, del HSV-2 (ICP22-deficient HSV-2) replication is more sensitive to IFN-β treatment, indicating... More

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