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Genome-wide siRNA Screening at Biosafety Level 4 Reveals a Crucial Role for Fibrillarin in Henipavirus Infection

Hendra and Nipah viruses (genus Henipavirus, family Paramyxoviridae) are highly pathogenic bat-borne viruses. The need for high biocontainment when studying henipaviruses has hindered the development of therapeutics and knowledge of the viral infection cycle. We have performed a genome-wide siRNA sc...

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Autores principales: Deffrasnes, Celine, Marsh, Glenn A., Foo, Chwan Hong, Rootes, Christina L., Gould, Cathryn M., Grusovin, Julian, Monaghan, Paul, Lo, Michael K., Tompkins, S. Mark, Adams, Timothy E., Lowenthal, John W., Simpson, Kaylene J., Stewart, Cameron R., Bean, Andrew G. D., Wang, Lin-Fa
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4806981/
https://www.ncbi.nlm.nih.gov/pubmed/27010548
http://dx.doi.org/10.1371/journal.ppat.1005478
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author Deffrasnes, Celine
Marsh, Glenn A.
Foo, Chwan Hong
Rootes, Christina L.
Gould, Cathryn M.
Grusovin, Julian
Monaghan, Paul
Lo, Michael K.
Tompkins, S. Mark
Adams, Timothy E.
Lowenthal, John W.
Simpson, Kaylene J.
Stewart, Cameron R.
Bean, Andrew G. D.
Wang, Lin-Fa
author_facet Deffrasnes, Celine
Marsh, Glenn A.
Foo, Chwan Hong
Rootes, Christina L.
Gould, Cathryn M.
Grusovin, Julian
Monaghan, Paul
Lo, Michael K.
Tompkins, S. Mark
Adams, Timothy E.
Lowenthal, John W.
Simpson, Kaylene J.
Stewart, Cameron R.
Bean, Andrew G. D.
Wang, Lin-Fa
author_sort Deffrasnes, Celine
collection PubMed
description Hendra and Nipah viruses (genus Henipavirus, family Paramyxoviridae) are highly pathogenic bat-borne viruses. The need for high biocontainment when studying henipaviruses has hindered the development of therapeutics and knowledge of the viral infection cycle. We have performed a genome-wide siRNA screen at biosafety level 4 that identified 585 human proteins required for henipavirus infection. The host protein with the largest impact was fibrillarin, a nucleolar methyltransferase that was also required by measles, mumps and respiratory syncytial viruses for infection. While not required for cell entry, henipavirus RNA and protein syntheses were greatly impaired in cells lacking fibrillarin, indicating a crucial role in the RNA replication phase of infection. During infection, the Hendra virus matrix protein co-localized with fibrillarin in cell nucleoli, and co-associated as a complex in pulldown studies, while its nuclear import was unaffected in fibrillarin-depleted cells. Mutagenesis studies showed that the methyltransferase activity of fibrillarin was required for henipavirus infection, suggesting that this enzyme could be targeted therapeutically to combat henipavirus infections.
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spelling pubmed-48069812016-03-25 Genome-wide siRNA Screening at Biosafety Level 4 Reveals a Crucial Role for Fibrillarin in Henipavirus Infection Deffrasnes, Celine Marsh, Glenn A. Foo, Chwan Hong Rootes, Christina L. Gould, Cathryn M. Grusovin, Julian Monaghan, Paul Lo, Michael K. Tompkins, S. Mark Adams, Timothy E. Lowenthal, John W. Simpson, Kaylene J. Stewart, Cameron R. Bean, Andrew G. D. Wang, Lin-Fa PLoS Pathog Research Article Hendra and Nipah viruses (genus Henipavirus, family Paramyxoviridae) are highly pathogenic bat-borne viruses. The need for high biocontainment when studying henipaviruses has hindered the development of therapeutics and knowledge of the viral infection cycle. We have performed a genome-wide siRNA screen at biosafety level 4 that identified 585 human proteins required for henipavirus infection. The host protein with the largest impact was fibrillarin, a nucleolar methyltransferase that was also required by measles, mumps and respiratory syncytial viruses for infection. While not required for cell entry, henipavirus RNA and protein syntheses were greatly impaired in cells lacking fibrillarin, indicating a crucial role in the RNA replication phase of infection. During infection, the Hendra virus matrix protein co-localized with fibrillarin in cell nucleoli, and co-associated as a complex in pulldown studies, while its nuclear import was unaffected in fibrillarin-depleted cells. Mutagenesis studies showed that the methyltransferase activity of fibrillarin was required for henipavirus infection, suggesting that this enzyme could be targeted therapeutically to combat henipavirus infections. Public Library of Science 2016-03-24 /pmc/articles/PMC4806981/ /pubmed/27010548 http://dx.doi.org/10.1371/journal.ppat.1005478 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration, which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose.
spellingShingle Research Article
Deffrasnes, Celine
Marsh, Glenn A.
Foo, Chwan Hong
Rootes, Christina L.
Gould, Cathryn M.
Grusovin, Julian
Monaghan, Paul
Lo, Michael K.
Tompkins, S. Mark
Adams, Timothy E.
Lowenthal, John W.
Simpson, Kaylene J.
Stewart, Cameron R.
Bean, Andrew G. D.
Wang, Lin-Fa
Genome-wide siRNA Screening at Biosafety Level 4 Reveals a Crucial Role for Fibrillarin in Henipavirus Infection
title Genome-wide siRNA Screening at Biosafety Level 4 Reveals a Crucial Role for Fibrillarin in Henipavirus Infection
title_full Genome-wide siRNA Screening at Biosafety Level 4 Reveals a Crucial Role for Fibrillarin in Henipavirus Infection
title_fullStr Genome-wide siRNA Screening at Biosafety Level 4 Reveals a Crucial Role for Fibrillarin in Henipavirus Infection
title_full_unstemmed Genome-wide siRNA Screening at Biosafety Level 4 Reveals a Crucial Role for Fibrillarin in Henipavirus Infection
title_short Genome-wide siRNA Screening at Biosafety Level 4 Reveals a Crucial Role for Fibrillarin in Henipavirus Infection
title_sort genome-wide sirna screening at biosafety level 4 reveals a crucial role for fibrillarin in henipavirus infection
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4806981/
https://www.ncbi.nlm.nih.gov/pubmed/27010548
http://dx.doi.org/10.1371/journal.ppat.1005478
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