Literature DB >> 21502533

Identification of broad-spectrum antiviral compounds and assessment of the druggability of their target for efficacy against respiratory syncytial virus (RSV).

Aurelio Bonavia1, Michael Franti, Erin Pusateri Keaney, Kelli Kuhen, Mohindra Seepersaud, Branko Radetich, Jian Shao, Ayako Honda, Janetta Dewhurst, Kara Balabanis, James Monroe, Karen Wolff, Colin Osborne, Leanne Lanieri, Keith Hoffmaster, Jakal Amin, Judit Markovits, Michelle Broome, Elizabeth Skuba, Ivan Cornella-Taracido, Gerard Joberty, Tewis Bouwmeester, Lawrence Hamann, John A Tallarico, Ruben Tommasi, Teresa Compton, Simon M Bushell.   

Abstract

The search for novel therapeutic interventions for viral disease is a challenging pursuit, hallmarked by the paucity of antiviral agents currently prescribed. Targeting of viral proteins has the inextricable challenge of rise of resistance. Safe and effective vaccines are not possible for many viral pathogens. New approaches are required to address the unmet medical need in this area. We undertook a cell-based high-throughput screen to identify leads for development of drugs to treat respiratory syncytial virus (RSV), a serious pediatric pathogen. We identified compounds that are potent (nanomolar) inhibitors of RSV in vitro in HEp-2 cells and in primary human bronchial epithelial cells and were shown to act postentry. Interestingly, two scaffolds exhibited broad-spectrum activity among multiple RNA viruses. Using the chemical matter as a probe, we identified the targets and identified a common cellular pathway: the de novo pyrimidine biosynthesis pathway. Both targets were validated in vitro and showed no significant cell cytotoxicity except for activity against proliferative B- and T-type lymphoid cells. Corollary to this finding was to understand the consequences of inhibition of the target to the host. An in vivo assessment for antiviral efficacy failed to demonstrate reduced viral load, but revealed microscopic changes and a trend toward reduced pyrimidine pools and findings in histopathology. We present here a discovery program that includes screen, target identification, validation, and druggability that can be broadly applied to identify and interrogate other host factors for antiviral effect starting from chemical matter of unknown target/mechanism of action.

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Year:  2011        PMID: 21502533      PMCID: PMC3084118          DOI: 10.1073/pnas.1017142108

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  48 in total

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Review 7.  Bronchiolitis.

Authors:  Rosalind L Smyth; Peter J M Openshaw
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10.  Post-infection A77-1726 blocks pathophysiologic sequelae of respiratory syncytial virus infection.

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  39 in total

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Journal:  J Virol       Date:  2016-04-14       Impact factor: 5.103

2.  Quantitative proteomic analysis of host-virus interactions reveals a role for Golgi brefeldin A resistance factor 1 (GBF1) in dengue infection.

Authors:  Lindsay N Carpp; Richard S Rogers; Robert L Moritz; John D Aitchison
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3.  Metabolic Modifier Screen Reveals Secondary Targets of Protein Kinase Inhibitors within Nucleotide Metabolism.

Authors:  Evan R Abt; Ethan W Rosser; Matthew A Durst; Vincent Lok; Soumya Poddar; Thuc M Le; Arthur Cho; Woosuk Kim; Liu Wei; Janet Song; Joseph R Capri; Shili Xu; Nanping Wu; Roger Slavik; Michael E Jung; Robert Damoiseaux; Johannes Czernin; Timothy R Donahue; Arnon Lavie; Caius G Radu
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4.  Inhibition of dengue virus through suppression of host pyrimidine biosynthesis.

Authors:  Qing-Yin Wang; Simon Bushell; Min Qing; Hao Ying Xu; Aurelio Bonavia; Sandra Nunes; Jing Zhou; Mee Kian Poh; Paola Florez de Sessions; Pornwaratt Niyomrattanakit; Hongping Dong; Keith Hoffmaster; Anne Goh; Shahul Nilar; Wouter Schul; Susan Jones; Laura Kramer; Teresa Compton; Pei-Yong Shi
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5.  Inhibiting pyrimidine biosynthesis impairs Ebola virus replication through depletion of nucleoside pools and activation of innate immune responses.

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Journal:  Antiviral Res       Date:  2018-08-23       Impact factor: 5.970

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7.  Novel indole-2-carboxamide compounds are potent broad-spectrum antivirals active against western equine encephalitis virus in vivo.

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Journal:  J Virol       Date:  2014-07-16       Impact factor: 5.103

8.  Discovery of a Broad-Spectrum Antiviral Compound That Inhibits Pyrimidine Biosynthesis and Establishes a Type 1 Interferon-Independent Antiviral State.

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9.  JC Polyomavirus Attachment and Entry: Potential Sites for PML Therapeutics.

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Journal:  Curr Clin Microbiol Rep       Date:  2017-08-01

Review 10.  JC polyomavirus attachment, entry, and trafficking: unlocking the keys to a fatal infection.

Authors:  Melissa S Maginnis; Christian D S Nelson; Walter J Atwood
Journal:  J Neurovirol       Date:  2014-07-31       Impact factor: 2.643

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