PUL21a-Cyclin A2 Interaction is Required to Protect Human Cytomegalovirus-Infected Cells from the Deleterious Consequences of Mitotic Entry

Entry into mitosis is accompanied by dramatic changes in cellular architecture, metabolism and gene expression. Many viruses have evolved cell cycle arrest strategies to prevent mitotic entry, presumably to ensure sustained, uninterrupted viral replication. Here we show for human cytomegalovirus (HC...

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Autores principales: Eifler, Martin, Uecker, Ralf, Weisbach, Henry, Bogdanow, Boris, Richter, Ellen, König, Lydia, Vetter, Barbara, Lenac-Rovis, Tihana, Jonjic, Stipan, Neitzel, Heidemarie, Hagemeier, Christian, Wiebusch, Lüder
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4231158/
https://www.ncbi.nlm.nih.gov/pubmed/25393019
http://dx.doi.org/10.1371/journal.ppat.1004514
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author Eifler, Martin
Uecker, Ralf
Weisbach, Henry
Bogdanow, Boris
Richter, Ellen
König, Lydia
Vetter, Barbara
Lenac-Rovis, Tihana
Jonjic, Stipan
Neitzel, Heidemarie
Hagemeier, Christian
Wiebusch, Lüder
author_facet Eifler, Martin
Uecker, Ralf
Weisbach, Henry
Bogdanow, Boris
Richter, Ellen
König, Lydia
Vetter, Barbara
Lenac-Rovis, Tihana
Jonjic, Stipan
Neitzel, Heidemarie
Hagemeier, Christian
Wiebusch, Lüder
author_sort Eifler, Martin
collection PubMed
description Entry into mitosis is accompanied by dramatic changes in cellular architecture, metabolism and gene expression. Many viruses have evolved cell cycle arrest strategies to prevent mitotic entry, presumably to ensure sustained, uninterrupted viral replication. Here we show for human cytomegalovirus (HCMV) what happens if the viral cell cycle arrest mechanism is disabled and cells engaged in viral replication enter into unscheduled mitosis. We made use of an HCMV mutant that, due to a defective Cyclin A2 binding motif in its UL21a gene product (pUL21a), has lost its ability to down-regulate Cyclin A2 and, therefore, to arrest cells at the G1/S transition. Cyclin A2 up-regulation in infected cells not only triggered the onset of cellular DNA synthesis, but also promoted the accumulation and nuclear translocation of Cyclin B1-CDK1, premature chromatin condensation and mitotic entry. The infected cells were able to enter metaphase as shown by nuclear lamina disassembly and, often irregular, metaphase spindle formation. However, anaphase onset was blocked by the still intact anaphase promoting complex/cyclosome (APC/C) inhibitory function of pUL21a. Remarkably, the essential viral IE2, but not the related chromosome-associated IE1 protein, disappeared upon mitotic entry, suggesting an inherent instability of IE2 under mitotic conditions. Viral DNA synthesis was impaired in mitosis, as demonstrated by the abnormal morphology and strongly reduced BrdU incorporation rates of viral replication compartments. The prolonged metaphase arrest in infected cells coincided with precocious sister chromatid separation and progressive fragmentation of the chromosomal material. We conclude that the Cyclin A2-binding function of pUL21a contributes to the maintenance of a cell cycle state conducive for the completion of the HCMV replication cycle. Unscheduled mitotic entry during the course of the HCMV replication has fatal consequences, leading to abortive infection and cell death.
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spelling pubmed-42311582014-11-18 PUL21a-Cyclin A2 Interaction is Required to Protect Human Cytomegalovirus-Infected Cells from the Deleterious Consequences of Mitotic Entry Eifler, Martin Uecker, Ralf Weisbach, Henry Bogdanow, Boris Richter, Ellen König, Lydia Vetter, Barbara Lenac-Rovis, Tihana Jonjic, Stipan Neitzel, Heidemarie Hagemeier, Christian Wiebusch, Lüder PLoS Pathog Research Article Entry into mitosis is accompanied by dramatic changes in cellular architecture, metabolism and gene expression. Many viruses have evolved cell cycle arrest strategies to prevent mitotic entry, presumably to ensure sustained, uninterrupted viral replication. Here we show for human cytomegalovirus (HCMV) what happens if the viral cell cycle arrest mechanism is disabled and cells engaged in viral replication enter into unscheduled mitosis. We made use of an HCMV mutant that, due to a defective Cyclin A2 binding motif in its UL21a gene product (pUL21a), has lost its ability to down-regulate Cyclin A2 and, therefore, to arrest cells at the G1/S transition. Cyclin A2 up-regulation in infected cells not only triggered the onset of cellular DNA synthesis, but also promoted the accumulation and nuclear translocation of Cyclin B1-CDK1, premature chromatin condensation and mitotic entry. The infected cells were able to enter metaphase as shown by nuclear lamina disassembly and, often irregular, metaphase spindle formation. However, anaphase onset was blocked by the still intact anaphase promoting complex/cyclosome (APC/C) inhibitory function of pUL21a. Remarkably, the essential viral IE2, but not the related chromosome-associated IE1 protein, disappeared upon mitotic entry, suggesting an inherent instability of IE2 under mitotic conditions. Viral DNA synthesis was impaired in mitosis, as demonstrated by the abnormal morphology and strongly reduced BrdU incorporation rates of viral replication compartments. The prolonged metaphase arrest in infected cells coincided with precocious sister chromatid separation and progressive fragmentation of the chromosomal material. We conclude that the Cyclin A2-binding function of pUL21a contributes to the maintenance of a cell cycle state conducive for the completion of the HCMV replication cycle. Unscheduled mitotic entry during the course of the HCMV replication has fatal consequences, leading to abortive infection and cell death. Public Library of Science 2014-11-13 /pmc/articles/PMC4231158/ /pubmed/25393019 http://dx.doi.org/10.1371/journal.ppat.1004514 Text en © 2014 Eifler 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
Eifler, Martin
Uecker, Ralf
Weisbach, Henry
Bogdanow, Boris
Richter, Ellen
König, Lydia
Vetter, Barbara
Lenac-Rovis, Tihana
Jonjic, Stipan
Neitzel, Heidemarie
Hagemeier, Christian
Wiebusch, Lüder
PUL21a-Cyclin A2 Interaction is Required to Protect Human Cytomegalovirus-Infected Cells from the Deleterious Consequences of Mitotic Entry
title PUL21a-Cyclin A2 Interaction is Required to Protect Human Cytomegalovirus-Infected Cells from the Deleterious Consequences of Mitotic Entry
title_full PUL21a-Cyclin A2 Interaction is Required to Protect Human Cytomegalovirus-Infected Cells from the Deleterious Consequences of Mitotic Entry
title_fullStr PUL21a-Cyclin A2 Interaction is Required to Protect Human Cytomegalovirus-Infected Cells from the Deleterious Consequences of Mitotic Entry
title_full_unstemmed PUL21a-Cyclin A2 Interaction is Required to Protect Human Cytomegalovirus-Infected Cells from the Deleterious Consequences of Mitotic Entry
title_short PUL21a-Cyclin A2 Interaction is Required to Protect Human Cytomegalovirus-Infected Cells from the Deleterious Consequences of Mitotic Entry
title_sort pul21a-cyclin a2 interaction is required to protect human cytomegalovirus-infected cells from the deleterious consequences of mitotic entry
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4231158/
https://www.ncbi.nlm.nih.gov/pubmed/25393019
http://dx.doi.org/10.1371/journal.ppat.1004514
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