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The Replicative Consequences of Papillomavirus E2 Protein Binding to the Origin Replication Factor ORC2

The origin recognition complex (ORC) coordinates a series of events that lead to initiation of DNA strand duplication. As a nuclear double stranded DNA plasmid, the papillomavirus (PV) genome resembles a mini-chromosome in infected cells. To initiate its replication, the viral E2 protein binds to an...

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Autores principales: DeSmet, Marsha, Kanginakudru, Sriramana, Rietz, Anne, Wu, Wai-Hong, Roden, Richard, Androphy, Elliot J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5049798/
https://www.ncbi.nlm.nih.gov/pubmed/27701460
http://dx.doi.org/10.1371/journal.ppat.1005934
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author DeSmet, Marsha
Kanginakudru, Sriramana
Rietz, Anne
Wu, Wai-Hong
Roden, Richard
Androphy, Elliot J.
author_facet DeSmet, Marsha
Kanginakudru, Sriramana
Rietz, Anne
Wu, Wai-Hong
Roden, Richard
Androphy, Elliot J.
author_sort DeSmet, Marsha
collection PubMed
description The origin recognition complex (ORC) coordinates a series of events that lead to initiation of DNA strand duplication. As a nuclear double stranded DNA plasmid, the papillomavirus (PV) genome resembles a mini-chromosome in infected cells. To initiate its replication, the viral E2 protein binds to and recruits the E1 DNA helicase at the viral origin. PV genome replication program exhibits three stages: initial amplification from a single genome upon infection to a few copies per cell, a cell cycle linked maintenance phase, and a differentiation dependent late stage where the genome is amplified to thousands of copies. Involvement of ORC or other pre-replication complex (pre-RC) factors has not been described. We report that human PV (HPV) and bovine PV (BPV-1) E2 proteins bind to ORC2, however, ORC2 was not detected at the viral origin. Depletion of ORC2 enhanced PV replication in a transient replication model and in keratinocytes stably maintaining viral episomes, while there was no effect on copy number in a cell line with integrated HPV genomes. Consistent with this, occupancy of E1 and E2 at the viral origin increased following ORC2 silencing. These data imply that ORC2 is not necessary for activation of the PV origin by E1 and E2 but instead suppresses E2 replicative function. Furthermore, we observed that over-expression of HPV E2 decreased ORC2 occupation at two known mammalian origins of replication, suggesting that E2 restricts pre-ORC assembly that could otherwise compete for host replication complexes necessary for viral genome amplification. We infer that the ORC2 complex with E2 restricts viral replication in the maintenance phase of the viral replication program and that elevated levels of E2 that occur during the differentiation dependent amplification stage subvert ORC loading and hence DNA synthesis at cellular origins.
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spelling pubmed-50497982016-10-27 The Replicative Consequences of Papillomavirus E2 Protein Binding to the Origin Replication Factor ORC2 DeSmet, Marsha Kanginakudru, Sriramana Rietz, Anne Wu, Wai-Hong Roden, Richard Androphy, Elliot J. PLoS Pathog Research Article The origin recognition complex (ORC) coordinates a series of events that lead to initiation of DNA strand duplication. As a nuclear double stranded DNA plasmid, the papillomavirus (PV) genome resembles a mini-chromosome in infected cells. To initiate its replication, the viral E2 protein binds to and recruits the E1 DNA helicase at the viral origin. PV genome replication program exhibits three stages: initial amplification from a single genome upon infection to a few copies per cell, a cell cycle linked maintenance phase, and a differentiation dependent late stage where the genome is amplified to thousands of copies. Involvement of ORC or other pre-replication complex (pre-RC) factors has not been described. We report that human PV (HPV) and bovine PV (BPV-1) E2 proteins bind to ORC2, however, ORC2 was not detected at the viral origin. Depletion of ORC2 enhanced PV replication in a transient replication model and in keratinocytes stably maintaining viral episomes, while there was no effect on copy number in a cell line with integrated HPV genomes. Consistent with this, occupancy of E1 and E2 at the viral origin increased following ORC2 silencing. These data imply that ORC2 is not necessary for activation of the PV origin by E1 and E2 but instead suppresses E2 replicative function. Furthermore, we observed that over-expression of HPV E2 decreased ORC2 occupation at two known mammalian origins of replication, suggesting that E2 restricts pre-ORC assembly that could otherwise compete for host replication complexes necessary for viral genome amplification. We infer that the ORC2 complex with E2 restricts viral replication in the maintenance phase of the viral replication program and that elevated levels of E2 that occur during the differentiation dependent amplification stage subvert ORC loading and hence DNA synthesis at cellular origins. Public Library of Science 2016-10-04 /pmc/articles/PMC5049798/ /pubmed/27701460 http://dx.doi.org/10.1371/journal.ppat.1005934 Text en © 2016 DeSmet 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, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
DeSmet, Marsha
Kanginakudru, Sriramana
Rietz, Anne
Wu, Wai-Hong
Roden, Richard
Androphy, Elliot J.
The Replicative Consequences of Papillomavirus E2 Protein Binding to the Origin Replication Factor ORC2
title The Replicative Consequences of Papillomavirus E2 Protein Binding to the Origin Replication Factor ORC2
title_full The Replicative Consequences of Papillomavirus E2 Protein Binding to the Origin Replication Factor ORC2
title_fullStr The Replicative Consequences of Papillomavirus E2 Protein Binding to the Origin Replication Factor ORC2
title_full_unstemmed The Replicative Consequences of Papillomavirus E2 Protein Binding to the Origin Replication Factor ORC2
title_short The Replicative Consequences of Papillomavirus E2 Protein Binding to the Origin Replication Factor ORC2
title_sort replicative consequences of papillomavirus e2 protein binding to the origin replication factor orc2
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5049798/
https://www.ncbi.nlm.nih.gov/pubmed/27701460
http://dx.doi.org/10.1371/journal.ppat.1005934
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