Literature DB >> 19019822

Agonist and antagonist recognition by RIG-I, a cytoplasmic innate immunity receptor.

C T Ranjith-Kumar1, Ayaluru Murali, Wen Dong, Dharmaiah Srisathiyanarayanan, Robert Vaughan, Joanna Ortiz-Alacantara, Kanchan Bhardwaj, Xiaojun Li, Pingwei Li, Cheng C Kao.   

Abstract

Cytoplasmic RNA receptors are important in the detection of and response to viral infections. We analyzed ligand recognition by the retinoic acid-inducible protein I (RIG-I) protein in biochemical assays and in transiently transfected cells and characterized the requirements for both single- and double-stranded RNA agonists for RIG-I activation of signaling. RIG-I mutants such as K270A and T409A/S411A that were defective in signaling with triphosphorylated single-stranded RNAs were perfectly capable of signaling with dsRNAs. Furthermore, phosphorothioated oligodeoxynucleotides were found to antagonize RIG-I signaling. Both agonists and antagonist bind purified RIG-I protein and a truncated RIG-I protein that lacked the signaling domain. The agonists were necessary to activate RIG-I ATPase activity in vitro, whereas antagonist inhibited ATPase activity. Differential scanning fluorometry showed that RIG-I bound to agonists, and antagonists have different denaturation properties, suggesting a difference in protein conformations. Last, single particle reconstruction was used to generate three-dimensional models of the RIG-I dimers in complex with an agonist and an antagonist. The two complexes exhibited dramatically different structures.

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Year:  2008        PMID: 19019822      PMCID: PMC2613625          DOI: 10.1074/jbc.M806219200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


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