Interactions of Prototype Foamy Virus Capsids with Host Cell Polo-Like Kinases Are Important for Efficient Viral DNA Integration

Unlike for other retroviruses, only a few host cell factors that aid the replication of foamy viruses (FVs) via interaction with viral structural components are known. Using a yeast-two-hybrid (Y2H) screen with prototype FV (PFV) Gag protein as bait we identified human polo-like kinase 2 (hPLK2), a...

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Autores principales: Zurnic, Irena, Hütter, Sylvia, Rzeha, Ute, Stanke, Nicole, Reh, Juliane, Müllers, Erik, Hamann, Martin V., Kern, Tobias, Gerresheim, Gesche K., Lindel, Fabian, Serrao, Erik, Lesbats, Paul, Engelman, Alan N., Cherepanov, Peter, Lindemann, Dirk
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5006980/
https://www.ncbi.nlm.nih.gov/pubmed/27579920
http://dx.doi.org/10.1371/journal.ppat.1005860
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author Zurnic, Irena
Hütter, Sylvia
Rzeha, Ute
Stanke, Nicole
Reh, Juliane
Müllers, Erik
Hamann, Martin V.
Kern, Tobias
Gerresheim, Gesche K.
Lindel, Fabian
Serrao, Erik
Lesbats, Paul
Engelman, Alan N.
Cherepanov, Peter
Lindemann, Dirk
author_facet Zurnic, Irena
Hütter, Sylvia
Rzeha, Ute
Stanke, Nicole
Reh, Juliane
Müllers, Erik
Hamann, Martin V.
Kern, Tobias
Gerresheim, Gesche K.
Lindel, Fabian
Serrao, Erik
Lesbats, Paul
Engelman, Alan N.
Cherepanov, Peter
Lindemann, Dirk
author_sort Zurnic, Irena
collection PubMed
description Unlike for other retroviruses, only a few host cell factors that aid the replication of foamy viruses (FVs) via interaction with viral structural components are known. Using a yeast-two-hybrid (Y2H) screen with prototype FV (PFV) Gag protein as bait we identified human polo-like kinase 2 (hPLK2), a member of cell cycle regulatory kinases, as a new interactor of PFV capsids. Further Y2H studies confirmed interaction of PFV Gag with several PLKs of both human and rat origin. A consensus Ser-Thr/Ser-Pro (S-T/S-P) motif in Gag, which is conserved among primate FVs and phosphorylated in PFV virions, was essential for recognition by PLKs. In the case of rat PLK2, functional kinase and polo-box domains were required for interaction with PFV Gag. Fluorescently-tagged PFV Gag, through its chromatin tethering function, selectively relocalized ectopically expressed eGFP-tagged PLK proteins to mitotic chromosomes in a Gag STP motif-dependent manner, confirming a specific and dominant nature of the Gag-PLK interaction in mammalian cells. The functional relevance of the Gag-PLK interaction was examined in the context of replication-competent FVs and single-round PFV vectors. Although STP motif mutated viruses displayed wild type (wt) particle release, RNA packaging and intra-particle reverse transcription, their replication capacity was decreased 3-fold in single-cycle infections, and up to 20-fold in spreading infections over an extended time period. Strikingly similar defects were observed when cells infected with single-round wt Gag PFV vectors were treated with a pan PLK inhibitor. Analysis of entry kinetics of the mutant viruses indicated a post-fusion defect resulting in delayed and reduced integration, which was accompanied with an enhanced preference to integrate into heterochromatin. We conclude that interaction between PFV Gag and cellular PLK proteins is important for early replication steps of PFV within host cells.
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spelling pubmed-50069802016-09-27 Interactions of Prototype Foamy Virus Capsids with Host Cell Polo-Like Kinases Are Important for Efficient Viral DNA Integration Zurnic, Irena Hütter, Sylvia Rzeha, Ute Stanke, Nicole Reh, Juliane Müllers, Erik Hamann, Martin V. Kern, Tobias Gerresheim, Gesche K. Lindel, Fabian Serrao, Erik Lesbats, Paul Engelman, Alan N. Cherepanov, Peter Lindemann, Dirk PLoS Pathog Research Article Unlike for other retroviruses, only a few host cell factors that aid the replication of foamy viruses (FVs) via interaction with viral structural components are known. Using a yeast-two-hybrid (Y2H) screen with prototype FV (PFV) Gag protein as bait we identified human polo-like kinase 2 (hPLK2), a member of cell cycle regulatory kinases, as a new interactor of PFV capsids. Further Y2H studies confirmed interaction of PFV Gag with several PLKs of both human and rat origin. A consensus Ser-Thr/Ser-Pro (S-T/S-P) motif in Gag, which is conserved among primate FVs and phosphorylated in PFV virions, was essential for recognition by PLKs. In the case of rat PLK2, functional kinase and polo-box domains were required for interaction with PFV Gag. Fluorescently-tagged PFV Gag, through its chromatin tethering function, selectively relocalized ectopically expressed eGFP-tagged PLK proteins to mitotic chromosomes in a Gag STP motif-dependent manner, confirming a specific and dominant nature of the Gag-PLK interaction in mammalian cells. The functional relevance of the Gag-PLK interaction was examined in the context of replication-competent FVs and single-round PFV vectors. Although STP motif mutated viruses displayed wild type (wt) particle release, RNA packaging and intra-particle reverse transcription, their replication capacity was decreased 3-fold in single-cycle infections, and up to 20-fold in spreading infections over an extended time period. Strikingly similar defects were observed when cells infected with single-round wt Gag PFV vectors were treated with a pan PLK inhibitor. Analysis of entry kinetics of the mutant viruses indicated a post-fusion defect resulting in delayed and reduced integration, which was accompanied with an enhanced preference to integrate into heterochromatin. We conclude that interaction between PFV Gag and cellular PLK proteins is important for early replication steps of PFV within host cells. Public Library of Science 2016-08-31 /pmc/articles/PMC5006980/ /pubmed/27579920 http://dx.doi.org/10.1371/journal.ppat.1005860 Text en © 2016 Zurnic 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
Zurnic, Irena
Hütter, Sylvia
Rzeha, Ute
Stanke, Nicole
Reh, Juliane
Müllers, Erik
Hamann, Martin V.
Kern, Tobias
Gerresheim, Gesche K.
Lindel, Fabian
Serrao, Erik
Lesbats, Paul
Engelman, Alan N.
Cherepanov, Peter
Lindemann, Dirk
Interactions of Prototype Foamy Virus Capsids with Host Cell Polo-Like Kinases Are Important for Efficient Viral DNA Integration
title Interactions of Prototype Foamy Virus Capsids with Host Cell Polo-Like Kinases Are Important for Efficient Viral DNA Integration
title_full Interactions of Prototype Foamy Virus Capsids with Host Cell Polo-Like Kinases Are Important for Efficient Viral DNA Integration
title_fullStr Interactions of Prototype Foamy Virus Capsids with Host Cell Polo-Like Kinases Are Important for Efficient Viral DNA Integration
title_full_unstemmed Interactions of Prototype Foamy Virus Capsids with Host Cell Polo-Like Kinases Are Important for Efficient Viral DNA Integration
title_short Interactions of Prototype Foamy Virus Capsids with Host Cell Polo-Like Kinases Are Important for Efficient Viral DNA Integration
title_sort interactions of prototype foamy virus capsids with host cell polo-like kinases are important for efficient viral dna integration
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5006980/
https://www.ncbi.nlm.nih.gov/pubmed/27579920
http://dx.doi.org/10.1371/journal.ppat.1005860
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