AI Article Synopsis

  • Cytoplasmic RIG-I-like receptors (RLRs) in mammalian cells detect viral RNA to trigger an antiviral response and induce IFN-β, with MDA5 forming fibers along viral dsRNA to enhance this response.
  • LGP2, a unique RLR that does not have a signaling domain, aids MDA5 in fiber formation and activates MDA5 by inducing conformational changes that expose its signaling components, the CARDs.
  • The study shows that LGP2 serves as a crucial partner for MDA5, facilitating its activation and maintaining its active state even after the fibers dissociate, providing insights into how LGP2 regulates MDA5 during antiviral immune responses.

Article Abstract

Cytoplasmic RIG-I-like receptor (RLR) proteins in mammalian cells recognize viral RNA and initiate an antiviral response that results in IFN-β induction. Melanoma differentiation-associated protein 5 (MDA5) forms fibers along viral dsRNA and propagates an antiviral response via a signaling domain, the tandem CARD. The most enigmatic RLR, laboratory of genetics and physiology (LGP2), lacks the signaling domain but functions in viral sensing through cooperation with MDA5. However, it remains unclear how LGP2 coordinates fiber formation and subsequent MDA5 activation. We utilized biochemical and biophysical approaches to observe fiber formation and the conformation of MDA5. LGP2 facilitated MDA5 fiber assembly. LGP2 was incorporated into the fibers with an average inter-molecular distance of 32 nm, suggesting the formation of hetero-oligomers with MDA5. Furthermore, limited protease digestion revealed that LGP2 induces significant conformational changes on MDA5, promoting exposure of its CARDs. Although the fibers were efficiently dissociated by ATP hydrolysis, MDA5 maintained its active conformation to participate in downstream signaling. Our study demonstrated the coordinated actions of LGP2 and MDA5, where LGP2 acts as an MDA5 nucleator and requisite partner in the conversion of MDA5 to an active conformation. We revealed a mechanistic basis for LGP2-mediated regulation of MDA5 antiviral innate immune responses.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7672446PMC
http://dx.doi.org/10.1093/nar/gkaa935DOI Listing

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