| Literature DB >> 21642987 |
Andreas Pichlmair1, Caroline Lassnig, Carol-Ann Eberle, Maria W Górna, Christoph L Baumann, Thomas R Burkard, Tilmann Bürckstümmer, Adrijana Stefanovic, Sigurd Krieger, Keiryn L Bennett, Thomas Rülicke, Friedemann Weber, Jacques Colinge, Mathias Müller, Giulio Superti-Furga.
Abstract
Antiviral innate immunity relies on the recognition of microbial structures. One such structure is viral RNA that carries a triphosphate group on its 5' terminus (PPP-RNA). By an affinity proteomics approach with PPP-RNA as the 'bait', we found that the antiviral protein IFIT1 (interferon-induced protein with tetratricopeptide repeats 1) mediated binding of a larger protein complex containing other IFIT family members. IFIT1 bound PPP-RNA with nanomolar affinity and required the arginine at position 187 in a highly charged carboxy-terminal groove of the protein. In the absence of IFIT1, the growth and pathogenicity of viruses containing PPP-RNA was much greater. In contrast, IFIT proteins were dispensable for the clearance of pathogens that did not generate PPP-RNA. On the basis of this specificity and the great abundance of IFIT proteins after infection, we propose that the IFIT complex antagonizes viruses by sequestering specific viral nucleic acids.Entities:
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Year: 2011 PMID: 21642987 DOI: 10.1038/ni.2048
Source DB: PubMed Journal: Nat Immunol ISSN: 1529-2908 Impact factor: 25.606