Literature DB >> 23221558

Identification of a noncanonically transcribed subgenomic mRNA of infectious bronchitis virus and other gammacoronaviruses.

Kirsten Bentley1, Sarah May Keep, Maria Armesto, Paul Britton.   

Abstract

Coronavirus subgenomic mRNA (sgmRNA) synthesis occurs via a process of discontinuous transcription involving transcription regulatory sequences (TRSs) located in the 5' leader sequence (TRS-L) and upstream of each structural and group-specific gene (TRS-B). Several gammacoronaviruses including infectious bronchitis virus (IBV) contain a putative open reading frame (ORF), localized between the M gene and gene 5, which is controversial due to the perceived absence of a TRS. We have studied the transcription of a novel sgmRNA associated with this potential ORF and found it to be transcribed via a previously unidentified noncanonical TRS-B. Using an IBV reverse genetics system, we demonstrated that the template-switching event during intergenic region (IR) sgmRNA synthesis occurs at the 5' end of the noncanonical TRS-B and recombines between nucleotides 5 and 6 of the 8-nucleotide consensus TRS-L. Introduction of a complete TRS-B showed that higher transcription levels are achieved by increasing the number of nucleotide matches between TRS-L and TRS-B. Translation of a protein from the sgmRNA was demonstrated using enhanced green fluorescent protein, suggesting the translation of a fifth, novel, group-specific protein for IBV. This study has resolved an issue concerning the number of ORFs expressed by members of the Gammacoronavirus genus and proposes the existence of a fifth IBV accessory protein. We confirmed previous reports that coronaviruses can produce sgmRNAs from noncanonical TRS-Bs, which may expand their repertoire of proteins. We also demonstrated that noncanonical TRS-Bs may provide a mechanism by which coronaviruses can control protein expression levels by reducing sgmRNA synthesis.

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Year:  2012        PMID: 23221558      PMCID: PMC3571483          DOI: 10.1128/JVI.02967-12

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


  41 in total

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3.  Severe acute respiratory syndrome coronavirus group-specific open reading frames encode nonessential functions for replication in cell cultures and mice.

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Journal:  J Virol       Date:  2005-12       Impact factor: 5.103

4.  Identification of novel subgenomic RNAs and noncanonical transcription initiation signals of severe acute respiratory syndrome coronavirus.

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5.  Structure and functional relevance of a transcription-regulating sequence involved in coronavirus discontinuous RNA synthesis.

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5.  A reverse genetics system for avian coronavirus infectious bronchitis virus based on targeted RNA recombination.

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6.  Complete genome analysis of Iranian IS-1494 like avian infectious bronchitis virus.

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7.  Infectious Bronchitis Virus as a Vector for the Expression of Heterologous Genes.

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8.  Identification of Amino Acids within Nonstructural Proteins 10 and 14 of the Avian Coronavirus Infectious Bronchitis Virus That Result in Attenuation In Vivo and In Ovo.

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9.  Genetic Characterization of the Belgian Nephropathogenic Infectious Bronchitis Virus (NIBV) Reference Strain B1648.

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10.  New insights about the regulation of Nidovirus subgenomic mRNA synthesis.

Authors:  Han Di; Ayisha A McIntyre; Margo A Brinton
Journal:  Virology       Date:  2018-02-21       Impact factor: 3.616

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