Literature DB >> 7769678

The antiviral compound enviroxime targets the 3A coding region of rhinovirus and poliovirus.

B A Heinz1, L M Vance.   

Abstract

Enviroxime is an antiviral compound that inhibits the replication of rhinoviruses and enteroviruses. We have explored the mechanism of action of enviroxime by using poliovirus type 1 and human rhinovirus type 14 as model systems. By varying the time of drug addition to virus-infected cells, we determined that enviroxime could be added several hours postinfection without significant loss of inhibition. This suggested that the drug targeted a step involved in RNA replication or protein processing. To identify this target, we mapped 23 independent mutations in mutants that could multiply in the presence of 1 microgram of enviroxime per ml. Each of these mutants contained a single nucleotide substitution that altered one amino acid in the 3A coding region. Using oligonucleotide-directed mutagenesis of cDNA clones, we have confirmed that these single-amino-acid substitutions are sufficient to confer the resistance phenotype. In addition, we conducted two experiments to support the hypothesis that enviroxime inhibits a 3A function. First, we determined by dot blot analysis of RNA from poliovirus-infected cells that enviroxime preferentially inhibits synthesis of the viral plus strand. Second, we demonstrated that enviroxime inhibits the initiation of plus-strand RNA synthesis as measured by the addition of [32P]uridine to 3AB in poliovirus crude replication complexes. To our knowledge, this is the first evidence that 3A can be targeted by antiviral drugs. We anticipate that enviroxime will be a useful tool for investigating the natural function of the 3A protein.

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Year:  1995        PMID: 7769678      PMCID: PMC189156          DOI: 10.1128/JVI.69.7.4189-4197.1995

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  67 in total

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3.  Genetic and molecular analyses of spontaneous mutants of human rhinovirus 14 that are resistant to an antiviral compound.

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4.  Mutational analysis of the genome-linked protein VPg of poliovirus.

Authors:  R J Kuhn; H Tada; M F Ypma-Wong; B L Semler; E Wimmer
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6.  A membrane-associated precursor to poliovirus VPg identified by immunoprecipitation with antibodies directed against a synthetic heptapeptide.

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7.  Prophylactic activity of intranasal enviroxime against experimentally induced rhinovirus type 39 infection.

Authors:  F G Hayden; J M Gwaltney
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Review 8.  Rapid evolution of RNA genomes.

Authors:  J Holland; K Spindler; F Horodyski; E Grabau; S Nichol; S VandePol
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10.  Phospholipid biosynthesis and poliovirus genome replication, two coupled phenomena.

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  41 in total

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4.  Mutations in the nonstructural protein 3A confer resistance to the novel enterovirus replication inhibitor TTP-8307.

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Review 6.  Molecular typing of enteroviruses: current status and future requirements. The European Union Concerted Action on Virus Meningitis and Encephalitis.

Authors:  P Muir; U Kämmerer; K Korn; M N Mulders; T Pöyry; B Weissbrich; R Kandolf; G M Cleator; A M van Loon
Journal:  Clin Microbiol Rev       Date:  1998-01       Impact factor: 26.132

7.  Sequence determinants of 3A-mediated resistance to enviroxime in rhinoviruses and enteroviruses.

Authors:  B A Heinz; L M Vance
Journal:  J Virol       Date:  1996-07       Impact factor: 5.103

8.  Reversible dissociation of the poliovirus replication complex: functions and interactions of its components in viral RNA synthesis.

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9.  Simple in vitro translation assay to analyze inhibitors of rhinovirus proteases.

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10.  In vitro activity of expanded-spectrum pyridazinyl oxime ethers related to pirodavir: novel capsid-binding inhibitors with potent antipicornavirus activity.

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