4.8 Article

5′-triphosphate RNA requires base-paired structures to activate antiviral signaling via RIG-I

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.0900971106

Keywords

immunostimulatory RNA; melanoma differentiation-associated protein 5; retinoid acid-inducible gene-I-like helicases; virus infection; interferon production

Funding

  1. Deutsche Forschungsgemeinschaft [DFGRO 2525/3-1, DFGGK 1202]
  2. LMUexcellent
  3. Sonderforschungsbereich [TR 36, EN 169/7-2]

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The ATPase retinoid acid-inducible gene (RIG)-I senses viral RNA in the cytoplasm of infected cells and subsequently activates cellular antiviral defense mechanisms. RIG-I recognizes molecular structures that discriminate viral from host RNA. Here, we show that RIG-I ligands require base-paired structures in conjunction with a free 5'-triphosphate to trigger antiviral signaling. Hitherto unavailable chemically synthesized 5'-triphosphate RNA ligands do not trigger RIG-I-dependent IFN production in cells, and they are unable to trigger the ATPase activity of RIG-I without a base-paired stretch. Consistently, immunostimulatory RNA from cells infected with a virus recognized by RIG-I is sensitive to double-strand, but not single-strand, specific RNases. In vitro, base-paired stretches and the 5'-triphosphate bind to distinct sites of RIG-I and synergize to trigger the induction of signaling competent RIG-I multimers. Strengthening our model of a bipartite molecular pattern for RIG-I activation, we show that the activity of supposedly single-stranded 5'-triphosphate RNAs generated by in vitro transcription depends on extended and base-paired by-products inadvertently, but commonly, produced by this method. Together, our findings accurately define a minimal molecular pattern sufficient to activate RIG-I that can be found in viral genomes or transcripts.

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