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The adenovirus major core protein VII is dispensable for virion assembly but is essential for lytic infection

The Adenovirus (Ad) genome within the capsid is tightly associated with a virus-encoded, histone-like core protein—protein VII. Two other Ad core proteins, V and X/μ, also are located within the virion and are loosely associated with viral DNA. Core protein VII remains associated with the Ad genome...

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Autores principales: Ostapchuk, Philomena, Suomalainen, Maarit, Zheng, Yueting, Boucke, Karin, Greber, Urs F., Hearing, Patrick
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5491326/
https://www.ncbi.nlm.nih.gov/pubmed/28628648
http://dx.doi.org/10.1371/journal.ppat.1006455
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author Ostapchuk, Philomena
Suomalainen, Maarit
Zheng, Yueting
Boucke, Karin
Greber, Urs F.
Hearing, Patrick
author_facet Ostapchuk, Philomena
Suomalainen, Maarit
Zheng, Yueting
Boucke, Karin
Greber, Urs F.
Hearing, Patrick
author_sort Ostapchuk, Philomena
collection PubMed
description The Adenovirus (Ad) genome within the capsid is tightly associated with a virus-encoded, histone-like core protein—protein VII. Two other Ad core proteins, V and X/μ, also are located within the virion and are loosely associated with viral DNA. Core protein VII remains associated with the Ad genome during the early phase of infection. It is not known if naked Ad DNA is packaged into the capsid, as with dsDNA bacteriophage and herpesviruses, followed by the encapsidation of viral core proteins, or if a unique packaging mechanism exists with Ad where a DNA-protein complex is simultaneously packaged into the virion. The latter model would require an entirely new molecular mechanism for packaging compared to known viral packaging motors. We characterized a virus with a conditional knockout of core protein VII. Remarkably, virus particles were assembled efficiently in the absence of protein VII. No changes in protein composition were evident with VII(−)virus particles, including the abundance of core protein V, but changes in the proteolytic processing of some capsid proteins were evident. Virus particles that lack protein VII enter the cell, but incoming virions did not escape efficiently from endosomes. This greatly diminished all subsequent aspects of the infectious cycle. These results reveal that the Ad major core protein VII is not required to condense viral DNA within the capsid, but rather plays an unexpected role during virus maturation and the early stages of infection. These results establish a new paradigm pertaining to the Ad assembly mechanism and reveal a new and important role of protein VII in early stages of infection.
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spelling pubmed-54913262017-07-18 The adenovirus major core protein VII is dispensable for virion assembly but is essential for lytic infection Ostapchuk, Philomena Suomalainen, Maarit Zheng, Yueting Boucke, Karin Greber, Urs F. Hearing, Patrick PLoS Pathog Research Article The Adenovirus (Ad) genome within the capsid is tightly associated with a virus-encoded, histone-like core protein—protein VII. Two other Ad core proteins, V and X/μ, also are located within the virion and are loosely associated with viral DNA. Core protein VII remains associated with the Ad genome during the early phase of infection. It is not known if naked Ad DNA is packaged into the capsid, as with dsDNA bacteriophage and herpesviruses, followed by the encapsidation of viral core proteins, or if a unique packaging mechanism exists with Ad where a DNA-protein complex is simultaneously packaged into the virion. The latter model would require an entirely new molecular mechanism for packaging compared to known viral packaging motors. We characterized a virus with a conditional knockout of core protein VII. Remarkably, virus particles were assembled efficiently in the absence of protein VII. No changes in protein composition were evident with VII(−)virus particles, including the abundance of core protein V, but changes in the proteolytic processing of some capsid proteins were evident. Virus particles that lack protein VII enter the cell, but incoming virions did not escape efficiently from endosomes. This greatly diminished all subsequent aspects of the infectious cycle. These results reveal that the Ad major core protein VII is not required to condense viral DNA within the capsid, but rather plays an unexpected role during virus maturation and the early stages of infection. These results establish a new paradigm pertaining to the Ad assembly mechanism and reveal a new and important role of protein VII in early stages of infection. Public Library of Science 2017-06-19 /pmc/articles/PMC5491326/ /pubmed/28628648 http://dx.doi.org/10.1371/journal.ppat.1006455 Text en © 2017 Ostapchuk et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Ostapchuk, Philomena
Suomalainen, Maarit
Zheng, Yueting
Boucke, Karin
Greber, Urs F.
Hearing, Patrick
The adenovirus major core protein VII is dispensable for virion assembly but is essential for lytic infection
title The adenovirus major core protein VII is dispensable for virion assembly but is essential for lytic infection
title_full The adenovirus major core protein VII is dispensable for virion assembly but is essential for lytic infection
title_fullStr The adenovirus major core protein VII is dispensable for virion assembly but is essential for lytic infection
title_full_unstemmed The adenovirus major core protein VII is dispensable for virion assembly but is essential for lytic infection
title_short The adenovirus major core protein VII is dispensable for virion assembly but is essential for lytic infection
title_sort adenovirus major core protein vii is dispensable for virion assembly but is essential for lytic infection
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5491326/
https://www.ncbi.nlm.nih.gov/pubmed/28628648
http://dx.doi.org/10.1371/journal.ppat.1006455
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