| Literature DB >> 29706547 |
Minghong Jiang1, Shikun Zhang1, Zongheng Yang1, Hongyu Lin1, Jun Zhu1, Lun Liu1, Wendie Wang1, Shuo Liu1, Wei Liu1, Yuanwu Ma2, Lianfeng Zhang2, Xuetao Cao3.
Abstract
The innate RNA sensor RIG-I is critical in the initiation of antiviral type I interferons (IFNs) production upon recognition of "non-self" viral RNAs. Here, we identify a host-derived, IFN-inducible long noncoding RNA, lnc-Lsm3b, that can compete with viral RNAs in the binding of RIG-I monomers and feedback inactivate the RIG-I innate function at late stage of innate response. Mechanistically, binding of lnc-Lsm3b restricts RIG-I protein's conformational shift and prevents downstream signaling, thereby terminating type I IFNs production. Multivalent structural motifs and long-stem structure are critical features of lnc-Lsm3b for RIG-I binding and inhibition. These data reveal a non-canonical self-recognition mode in the regulation of immune response and demonstrate an important role of an inducible "self" lncRNA acting as a potent molecular decoy actively saturating RIG-I binding sites to restrict the duration of "non-self" RNA-induced innate immune response and maintaining immune homeostasis, with potential utility in inflammatory disease management.Entities:
Keywords: RIG-I; immune homeostasis; innate immunity; lncRNA; non-self RNA; pathogenic dsRNA; self regulation; type I interferons
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Year: 2018 PMID: 29706547 DOI: 10.1016/j.cell.2018.03.064
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582