| Literature DB >> 29106386 |
Emily P Thi1, Chad E Mire2,3, Amy Ch Lee1, Joan B Geisbert2,3, Raul Ursic-Bedoya1, Krystle N Agans2,3, Marjorie Robbins1, Daniel J Deer2,3, Robert W Cross2,3, Andrew S Kondratowicz1, Karla A Fenton2,3, Ian MacLachlan1, Thomas W Geisbert2,3.
Abstract
Ebolaviruses and marburgviruses belong to the family Filoviridae and cause high lethality in infected patients. There are currently no licensed filovirus vaccines or antiviral therapies. The development of broad-spectrum therapies against members of the Marburgvirus genus, including Marburg virus (MARV) and Ravn virus (RAVV), is difficult because of substantial sequence variability. RNAi therapeutics offer a potential solution, as identification of conserved target nucleotide sequences may confer activity across marburgvirus variants. Here, we assessed the therapeutic efficacy of lipid nanoparticle (LNP) delivery of a single nucleoprotein-targeting (NP-targeting) siRNA in nonhuman primates at advanced stages of MARV or RAVV disease to mimic cases in which patients begin treatment for fulminant disease. Sixteen rhesus monkeys were lethally infected with MARV or RAVV and treated with NP siRNA-LNP, with MARV-infected animals beginning treatment four or five days after infection and RAVV-infected animals starting treatment three or six days after infection. While all untreated animals succumbed to disease, NP siRNA-LNP treatment conferred 100% survival of RAVV-infected macaques, even when treatment began just 1 day prior to the death of the control animals. In MARV-infected animals, day-4 treatment initiation resulted in 100% survival, and day-5 treatment resulted in 50% survival. These results identify a single siRNA therapeutic that provides broad-spectrum protection against both MARV and RAVV.Entities:
Keywords: Drug therapy; Infectious disease; Virology
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Year: 2017 PMID: 29106386 PMCID: PMC5707162 DOI: 10.1172/JCI96185
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808