| Literature DB >> 31533029 |
Courtney Woolsey1, Andrea R Menicucci2, Robert W Cross1, Priya Luthra3, Krystle N Agans1, Viktoriya Borisevich1, Joan B Geisbert1, Chad E Mire1, Karla A Fenton1, Allen Jankeel2, Sneha Anand2, Hideki Ebihara4, Thomas W Geisbert5, Ilhem Messaoudi6, Christopher F Basler7.
Abstract
Zaire ebolavirus (EBOV) VP35 protein is a suppressor of type I interferon (IFN) production, an inhibitor of dendritic cell maturation, and a putative virulence determinant. Here, a recombinant EBOV encoding a mutant VP35 virus (VP35m) is demonstrated to activate RIG-I-like receptor signaling and innate antiviral pathways. When inoculated into cynomolgus macaques, VP35m exhibits dramatic attenuation as compared to wild-type EBOV (wtEBOV), with 20 or 300 times the standard 100% lethal challenge dose not causing EBOV disease (EVD). Further, VP35m infection, despite limited replication in vivo, activates antigen presentation and innate immunity pathways and elicits increased frequencies of proliferating memory T cells and B cells and production of anti-EBOV antibodies. Upon wtEBOV challenge, VP35m-immunized animals survive, exhibiting host responses consistent with an orderly immune response and the absence of excessive inflammation. These data demonstrate that VP35 is a critical EBOV immune evasion factor and provide insights into immune mechanisms of EBOV control.Entities:
Keywords: Ebola; RIG-I; RLR signaling; VP35; filovirus; innate immunity; interferon; pathogenesis; primate
Year: 2019 PMID: 31533029 PMCID: PMC6886687 DOI: 10.1016/j.celrep.2019.08.047
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423