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Incoming RNA virus nucleocapsids containing a 5'-triphosphorylated genome activate RIG-I and antiviral signaling.

Cell host & microbe (2013-03-19)
Michaela Weber, Ali Gawanbacht, Matthias Habjan, Andreas Rang, Christoph Borner, Anna Mareike Schmidt, Sophie Veitinger, Ralf Jacob, Stéphanie Devignot, Georg Kochs, Adolfo García-Sastre, Friedemann Weber
RÉSUMÉ

Host defense to RNA viruses depends on rapid intracellular recognition of viral RNA by two cytoplasmic RNA helicases: RIG-I and MDA5. RNA transfection experiments indicate that RIG-I responds to naked double-stranded RNAs (dsRNAs) with a triphosphorylated 5' (5'ppp) terminus. However, the identity of the RIG-I stimulating viral structures in an authentic infection context remains unresolved. We show that incoming viral nucleocapsids containing a 5'ppp dsRNA "panhandle" structure trigger antiviral signaling that commences with RIG-I, is mediated through the adaptor protein MAVS, and terminates with transcription factor IRF-3. Independent of mammalian cofactors or viral polymerase activity, RIG-I bound to viral nucleocapsids, underwent a conformational switch, and homo-oligomerized. Enzymatic probing and superresolution microscopy suggest that RIG-I interacts with the panhandle structure of the viral nucleocapsids. These results define cytoplasmic entry of nucleocapsids as the proximal RIG-I-sensitive step during infection and establish viral nucleocapsids with a 5'ppp dsRNA panhandle as a RIG-I activator.

MATÉRIAUX
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Description du produit

Sigma-Aldrich
Sodium tripolyphosphate, technical grade, 85%
Sigma-Aldrich
Sodium triphosphate pentabasic, purum p.a., ≥98.0% (T)