Literature DB >> 21047962

The hydrophobic domain of infectious bronchitis virus E protein alters the host secretory pathway and is important for release of infectious virus.

Travis R Ruch1, Carolyn E Machamer.   

Abstract

The coronavirus (CoV) E protein plays an important role in virus assembly. The E protein is made in excess during infection and has been shown to have ion channel activity in planar lipid bilayers. However, a role in infection for the unincorporated E or its ion channel activity has not been described. To further investigate the function of the infectious bronchitis virus (IBV) E protein, we developed a recombinant version of IBV in which the E protein was replaced by a mutant containing a heterologous hydrophobic domain. The mutant virus, IBV-EG3, was defective in release of infectious virus particles. Further characterization of IBV-EG3 revealed that damaged particles appeared to accumulate intracellularly. The phenotype of IBV-EG3 suggested that the hydrophobic domain of IBV E may be important for the forward trafficking of cargo, so we determined whether IBV E facilitated the delivery of cargo to the plasma membrane. Surprisingly, we found that IBV E, but not EG3, dramatically reduced the delivery of cargo to the plasma membrane by impeding movement through the Golgi complex. Furthermore, we observed that overexpression of IBV E, but not EG3, induced the disassembly of the Golgi complex. Finally, we determined that the delivery of IBV S to the plasma membrane was reduced in cells infected with wild-type-IBV compared to those infected with IBV-EG3. Our results indicated that the hydrophobic domain of IBV E alters the host secretory pathway to the apparent advantage of the virus.

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Year:  2010        PMID: 21047962      PMCID: PMC3020032          DOI: 10.1128/JVI.01570-10

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


  40 in total

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Authors:  E Corse; C E Machamer
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6.  Influenza virus M2 protein has ion channel activity.

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7.  Specific structural alteration of the influenza haemagglutinin by amantadine.

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Authors:  J R Turner; A M Tartakoff
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  42 in total

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3.  Self-assembly of a nine-residue amyloid-forming peptide fragment of SARS corona virus E-protein: mechanism of self aggregation and amyloid-inhibition of hIAPP.

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4.  A Coronavirus E Protein Is Present in Two Distinct Pools with Different Effects on Assembly and the Secretory Pathway.

Authors:  Jason W Westerbeck; Carolyn E Machamer
Journal:  J Virol       Date:  2015-07-01       Impact factor: 5.103

5.  Identification of a Golgi complex-targeting signal in the cytoplasmic tail of the severe acute respiratory syndrome coronavirus envelope protein.

Authors:  Jennifer R Cohen; Lisa D Lin; Carolyn E Machamer
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Review 6.  Coronavirus pathogenesis.

Authors:  Susan R Weiss; Julian L Leibowitz
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7.  Analyses of Coronavirus Assembly Interactions with Interspecies Membrane and Nucleocapsid Protein Chimeras.

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Review 8.  The coronavirus E protein: assembly and beyond.

Authors:  Travis R Ruch; Carolyn E Machamer
Journal:  Viruses       Date:  2012-03-08       Impact factor: 5.048

9.  Coronavirus E protein forms ion channels with functionally and structurally-involved membrane lipids.

Authors:  Carmina Verdiá-Báguena; Jose L Nieto-Torres; Antonio Alcaraz; Marta L DeDiego; Jaume Torres; Vicente M Aguilella; Luis Enjuanes
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10.  A single polar residue and distinct membrane topologies impact the function of the infectious bronchitis coronavirus E protein.

Authors:  Travis R Ruch; Carolyn E Machamer
Journal:  PLoS Pathog       Date:  2012-05-03       Impact factor: 6.823

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