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Novel Polyomaviruses in Mammals from Multiple Orders and Reassessment of Polyomavirus Evolution and Taxonomy

As the phylogenetic organization of mammalian polyomaviruses is complex and currently incompletely resolved, we aimed at a deeper insight into their evolution by identifying polyomaviruses in host orders and families that have either rarely or not been studied. Sixteen unknown and two known polyomav...

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Autores principales: Ehlers, Bernhard, Anoh, Augustin E., Ben Salem, Nicole, Broll, Sebastian, Couacy-Hymann, Emmanuel, Fischer, Daniela, Gedvilaite, Alma, Ingenhütt, Nanina, Liebmann, Sonja, Martin, Maite, Mossoun, Arsene, Mugisha, Lawrence, Muyembe-Tamfum, Jean-Jacques, Pauly, Maude, Pérez de Val, Bernat, Preugschas, Hannah, Richter, Dania, Schubert, Grit, Szentiks, Claudia A., Teichmann, Tamara, Walter, Cornelia, Ulrich, Rainer G., Wiersma, Lidewij, Leendertz, Fabian H., Calvignac-Spencer, Sébastien
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6833039/
https://www.ncbi.nlm.nih.gov/pubmed/31658738
http://dx.doi.org/10.3390/v11100930
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author Ehlers, Bernhard
Anoh, Augustin E.
Ben Salem, Nicole
Broll, Sebastian
Couacy-Hymann, Emmanuel
Fischer, Daniela
Gedvilaite, Alma
Ingenhütt, Nanina
Liebmann, Sonja
Martin, Maite
Mossoun, Arsene
Mugisha, Lawrence
Muyembe-Tamfum, Jean-Jacques
Pauly, Maude
Pérez de Val, Bernat
Preugschas, Hannah
Richter, Dania
Schubert, Grit
Szentiks, Claudia A.
Teichmann, Tamara
Walter, Cornelia
Ulrich, Rainer G.
Wiersma, Lidewij
Leendertz, Fabian H.
Calvignac-Spencer, Sébastien
author_facet Ehlers, Bernhard
Anoh, Augustin E.
Ben Salem, Nicole
Broll, Sebastian
Couacy-Hymann, Emmanuel
Fischer, Daniela
Gedvilaite, Alma
Ingenhütt, Nanina
Liebmann, Sonja
Martin, Maite
Mossoun, Arsene
Mugisha, Lawrence
Muyembe-Tamfum, Jean-Jacques
Pauly, Maude
Pérez de Val, Bernat
Preugschas, Hannah
Richter, Dania
Schubert, Grit
Szentiks, Claudia A.
Teichmann, Tamara
Walter, Cornelia
Ulrich, Rainer G.
Wiersma, Lidewij
Leendertz, Fabian H.
Calvignac-Spencer, Sébastien
author_sort Ehlers, Bernhard
collection PubMed
description As the phylogenetic organization of mammalian polyomaviruses is complex and currently incompletely resolved, we aimed at a deeper insight into their evolution by identifying polyomaviruses in host orders and families that have either rarely or not been studied. Sixteen unknown and two known polyomaviruses were identified in animals that belong to 5 orders, 16 genera, and 16 species. From 11 novel polyomaviruses, full genomes could be determined. Splice sites were predicted for large and small T antigen (LTAg, STAg) coding sequences (CDS) and examined experimentally in transfected cell culture. In addition, splice sites of seven published polyomaviruses were analyzed. Based on these data, LTAg and STAg annotations were corrected for 10/86 and 74/86 published polyomaviruses, respectively. For 25 polyomaviruses, a spliced middle T CDS was observed or predicted. Splice sites that likely indicate expression of additional, alternative T antigens, were experimentally detected for six polyomaviruses. In contrast to all other mammalian polyomaviruses, three closely related cetartiodactyl polyomaviruses display two introns within their LTAg CDS. In addition, the VP2 of Glis glis (edible dormouse) polyomavirus 1 was observed to be encoded by a spliced transcript, a unique experimental finding within the Polyomaviridae family. Co-phylogenetic analyses based on LTAg CDS revealed a measurable signal of codivergence when considering all mammalian polyomaviruses, most likely driven by relatively recent codivergence events. Lineage duplication was the only other process whose influence on polyomavirus evolution was unambiguous. Finally, our analyses suggest that an update of the taxonomy of the family is required, including the creation of novel genera of mammalian and non-mammalian polyomaviruses.
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spelling pubmed-68330392019-11-25 Novel Polyomaviruses in Mammals from Multiple Orders and Reassessment of Polyomavirus Evolution and Taxonomy Ehlers, Bernhard Anoh, Augustin E. Ben Salem, Nicole Broll, Sebastian Couacy-Hymann, Emmanuel Fischer, Daniela Gedvilaite, Alma Ingenhütt, Nanina Liebmann, Sonja Martin, Maite Mossoun, Arsene Mugisha, Lawrence Muyembe-Tamfum, Jean-Jacques Pauly, Maude Pérez de Val, Bernat Preugschas, Hannah Richter, Dania Schubert, Grit Szentiks, Claudia A. Teichmann, Tamara Walter, Cornelia Ulrich, Rainer G. Wiersma, Lidewij Leendertz, Fabian H. Calvignac-Spencer, Sébastien Viruses Article As the phylogenetic organization of mammalian polyomaviruses is complex and currently incompletely resolved, we aimed at a deeper insight into their evolution by identifying polyomaviruses in host orders and families that have either rarely or not been studied. Sixteen unknown and two known polyomaviruses were identified in animals that belong to 5 orders, 16 genera, and 16 species. From 11 novel polyomaviruses, full genomes could be determined. Splice sites were predicted for large and small T antigen (LTAg, STAg) coding sequences (CDS) and examined experimentally in transfected cell culture. In addition, splice sites of seven published polyomaviruses were analyzed. Based on these data, LTAg and STAg annotations were corrected for 10/86 and 74/86 published polyomaviruses, respectively. For 25 polyomaviruses, a spliced middle T CDS was observed or predicted. Splice sites that likely indicate expression of additional, alternative T antigens, were experimentally detected for six polyomaviruses. In contrast to all other mammalian polyomaviruses, three closely related cetartiodactyl polyomaviruses display two introns within their LTAg CDS. In addition, the VP2 of Glis glis (edible dormouse) polyomavirus 1 was observed to be encoded by a spliced transcript, a unique experimental finding within the Polyomaviridae family. Co-phylogenetic analyses based on LTAg CDS revealed a measurable signal of codivergence when considering all mammalian polyomaviruses, most likely driven by relatively recent codivergence events. Lineage duplication was the only other process whose influence on polyomavirus evolution was unambiguous. Finally, our analyses suggest that an update of the taxonomy of the family is required, including the creation of novel genera of mammalian and non-mammalian polyomaviruses. MDPI 2019-10-10 /pmc/articles/PMC6833039/ /pubmed/31658738 http://dx.doi.org/10.3390/v11100930 Text en © 2019 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Ehlers, Bernhard
Anoh, Augustin E.
Ben Salem, Nicole
Broll, Sebastian
Couacy-Hymann, Emmanuel
Fischer, Daniela
Gedvilaite, Alma
Ingenhütt, Nanina
Liebmann, Sonja
Martin, Maite
Mossoun, Arsene
Mugisha, Lawrence
Muyembe-Tamfum, Jean-Jacques
Pauly, Maude
Pérez de Val, Bernat
Preugschas, Hannah
Richter, Dania
Schubert, Grit
Szentiks, Claudia A.
Teichmann, Tamara
Walter, Cornelia
Ulrich, Rainer G.
Wiersma, Lidewij
Leendertz, Fabian H.
Calvignac-Spencer, Sébastien
Novel Polyomaviruses in Mammals from Multiple Orders and Reassessment of Polyomavirus Evolution and Taxonomy
title Novel Polyomaviruses in Mammals from Multiple Orders and Reassessment of Polyomavirus Evolution and Taxonomy
title_full Novel Polyomaviruses in Mammals from Multiple Orders and Reassessment of Polyomavirus Evolution and Taxonomy
title_fullStr Novel Polyomaviruses in Mammals from Multiple Orders and Reassessment of Polyomavirus Evolution and Taxonomy
title_full_unstemmed Novel Polyomaviruses in Mammals from Multiple Orders and Reassessment of Polyomavirus Evolution and Taxonomy
title_short Novel Polyomaviruses in Mammals from Multiple Orders and Reassessment of Polyomavirus Evolution and Taxonomy
title_sort novel polyomaviruses in mammals from multiple orders and reassessment of polyomavirus evolution and taxonomy
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6833039/
https://www.ncbi.nlm.nih.gov/pubmed/31658738
http://dx.doi.org/10.3390/v11100930
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