Literature DB >> 25448087

Small molecule inhibitors of Ago2 decrease Venezuelan equine encephalitis virus replication.

Cathaleen Madsen1, Idris Hooper1, Lindsay Lundberg1, Nazly Shafagati1, Alexandra Johnson1, Svetlana Senina1, Cynthia de la Fuente1, Lisa I Hoover2, Brenda L Fredricksen2, Jonathan Dinman3, Jonathan L Jacobs4, Kylene Kehn-Hall5.   

Abstract

Venezuelan equine encephalitis virus (VEEV) is classified as a Category B Select Agent and potential bioterror weapon for its severe disease course in humans and equines and its potential for aerosol transmission. There are no current FDA licensed vaccines or specific therapies against VEEV, making identification of potential therapeutic targets a priority. With this aim, our research focuses on the interactions of VEEV with host microRNA (miRNA) machinery. miRNAs are small non-coding RNAs that act as master regulators of gene expression by downregulating or degrading messenger RNA, thus suppressing production of the resultant proteins. Recent publications implicate miRNA interactions in the pathogenesis of various viral diseases. To test the importance of miRNA processing for VEEV replication, cells deficient in Ago2, an important component of the RNA-induced silencing complex (RISC), and cells treated with known Ago2 inhibitors, notably acriflavine (ACF), were utilized. Both conditions caused decreased viral replication and capsid expression. ACF treatment promoted increased survival of neuronal cells over a non-treated, infected control and reduced viral titers of fully virulent VEEV as well as Eastern and Western Equine Encephalitis Viruses and West Nile Virus, but not Vesicular Stomatitis Virus. ACF treatment of VEEV TC-83 infected mice resulted in increased in vivo survival, but did not affect survival or viral loads when mice were challenged with fully virulent VEEV TrD. These results suggest that inhibition of Ago2 results in decreased replication of encephalitic alphaviruses in vitro and this pathway may be an avenue to explore for future therapeutic development.
Copyright © 2014 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Acriflavine; Ago2; Alphavirus; Therapeutic; Venezuelan equine encephalitis virus; miRNA

Mesh:

Substances:

Year:  2014        PMID: 25448087     DOI: 10.1016/j.antiviral.2014.10.002

Source DB:  PubMed          Journal:  Antiviral Res        ISSN: 0166-3542            Impact factor:   5.970


  11 in total

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6.  Synthesis and biological activity of conformationally restricted indole-based inhibitors of neurotropic alphavirus replication: Generation of a three-dimensional pharmacophore.

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7.  CpG and UpA dinucleotides in both coding and non-coding regions of echovirus 7 inhibit replication initiation post-entry.

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8.  Structure-guided screening strategy combining surface plasmon resonance with nuclear magnetic resonance for identification of small-molecule Argonaute 2 inhibitors.

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9.  Lipid-Coated Mesoporous Silica Nanoparticles for the Delivery of the ML336 Antiviral to Inhibit Encephalitic Alphavirus Infection.

Authors:  Annette E LaBauve; Torri E Rinker; Achraf Noureddine; Rita E Serda; Jane Y Howe; Michael B Sherman; Amy Rasley; C Jeffery Brinker; Darryl Y Sasaki; Oscar A Negrete
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Review 10.  A compendium of small molecule direct-acting and host-targeting inhibitors as therapies against alphaviruses.

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