Identification of a second binding site on the TRIM25 B30.2 domain

The etinoic acid- nducible ene- (RIG-I) receptor recognizes short 5'-di- and triphosphate base-paired viral RNA and is a critical mediator of the innate immune response against viruses such as influenza A, Ebola, HIV and hepatitis C. This response is reported to require an orchestrated interact...

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Published inBiochemical journal Vol. 475; no. 2; p. 429
Main Authors D'Cruz, Akshay A, Kershaw, Nadia J, Hayman, Thomas J, Linossi, Edmond M, Chiang, Jessica J, Wang, May K, Dagley, Laura F, Kolesnik, Tatiana B, Zhang, Jian-Guo, Masters, Seth L, Griffin, Michael D W, Gack, Michaela U, Murphy, James M, Nicola, Nicos A, Babon, Jeffrey J, Nicholson, Sandra E
Format Journal Article
LanguageEnglish
Published England 31.01.2018
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Summary:The etinoic acid- nducible ene- (RIG-I) receptor recognizes short 5'-di- and triphosphate base-paired viral RNA and is a critical mediator of the innate immune response against viruses such as influenza A, Ebola, HIV and hepatitis C. This response is reported to require an orchestrated interaction with the partite otif 25 (TRIM25) B30.2 protein-interaction domain. Here, we present a novel second RIG-I-binding interface on the TRIM25 B30.2 domain that interacts with CARD1 and CARD2 ( aspase ctivation and ecruitment omains) of RIG-I and is revealed by the removal of an N-terminal α-helix that mimics dimerization of the full-length protein. Further characterization of the TRIM25 coiled-coil and B30.2 regions indicated that the B30.2 domains move freely on a flexible tether, facilitating RIG-I CARD recruitment. The identification of a dual binding mode for the TRIM25 B30.2 domain is a first for the SPRY/B30.2 domain family and may be a feature of other SPRY/B30.2 family members.
ISSN:1470-8728
DOI:10.1042/BCJ20170427