1. Viral Double-Strand RNA-Binding Proteins Can Enhance Innate Immune Signaling by Toll-Like Receptor 3
- Author
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Kanchan Bhardwaj, Suchetana Mukhopadhyay, C. T. Ranjith-Kumar, Brady Tragesser, Guanghui Yi, Adam Zlotnick, Rodrigo A. Valverde, Yvonne Lai, Alice Chen, and C. Cheng Kao
- Subjects
Models, Molecular ,Protein Conformation ,viruses ,lcsh:Medicine ,RNA-binding protein ,Pathogenesis ,Plant Science ,Hepacivirus ,medicine.disease_cause ,Biochemistry ,Viral Packaging ,lcsh:Science ,Immune Response ,Polymerase ,0303 health sciences ,Toll-like receptor ,Multidisciplinary ,biology ,Viral Immune Evasion ,030302 biochemistry & molecular biology ,Viral Replication Complex ,RNA-Binding Proteins ,virus diseases ,hemic and immune systems ,Innate Immunity ,Enzymes ,3. Good health ,Host-Pathogen Interaction ,Protein Transport ,Viral Enzymes ,RNA, Viral ,Research Article ,Signal Transduction ,Genotype ,Hepatitis C virus ,Immunology ,RNA-dependent RNA polymerase ,chemical and pharmacologic phenomena ,Endosomes ,Viral Structure ,Microbiology ,Enzyme Regulation ,Immunomodulation ,Immune Activation ,Viral Proteins ,03 medical and health sciences ,Virology ,Viral Core ,Ross River virus ,medicine ,Viral Nucleic Acid ,Humans ,Nucleocapsid ,Biology ,Immunity to Infections ,RNA, Double-Stranded ,030304 developmental biology ,Inflammation ,Innate immune system ,lcsh:R ,Immunity ,Immunoregulation ,RNA ,Immune Defense ,Plant Pathology ,RNA-Dependent RNA Polymerase ,Viral Replication ,Immunity, Innate ,Toll-Like Receptor 3 ,HEK293 Cells ,Poly I-C ,Virulence Factors and Mechanisms ,TLR3 ,biology.protein ,Capsid Proteins ,lcsh:Q - Abstract
Toll-like Receptor 3 (TLR3) detects double-stranded (ds) RNAs to activate innate immune responses. While poly(I:C) is an excellent agonist for TLR3 in several cell lines and in human peripheral blood mononuclear cells, viral dsRNAs tend to be poor agonists, leading to the hypothesis that additional factor(s) are likely required to allow TLR3 to respond to viral dsRNAs. TLR3 signaling was examined in a lung epithelial cell line by quantifying cytokine production and in human embryonic kidney cells by quantifying luciferase reporter levels. Recombinant 1b hepatitis C virus polymerase was found to enhance TLR3 signaling in the lung epithelial BEAS-2B cells when added to the media along with either poly(I:C) or viral dsRNAs. The polymerase from the genotype 2a JFH-1 HCV was a poor enhancer of TLR3 signaling until it was mutated to favor a conformation that could bind better to a partially duplexed RNA. The 1b polymerase also co-localizes with TLR3 in endosomes. RNA-binding capsid proteins (CPs) from two positive-strand RNA viruses and the hepadenavirus hepatitis B virus (HBV) were also potent enhancers of TLR3 signaling by poly(I:C) or viral dsRNAs. A truncated version of the HBV CP that lacked an arginine-rich RNA-binding domain was unable to enhance TLR3 signaling. These results demonstrate that several viral RNA-binding proteins can enhance the dsRNA-dependent innate immune response initiated by TLR3.
- Published
- 2011
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