Ebola Virus Genome Plasticity as a Marker of Its Passaging History: A Comparison of In Vitro Passaging to Non-Human Primate Infection

To identify polymorphic sites that could be used as biomarkers of Ebola virus passage history, we repeatedly amplified Ebola virus (Kikwit variant) in vitro and in vivo and performed deep sequencing analysis of the complete genomes of the viral subpopulations. We then determined the sites undergoing...

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Autores principales: Kugelman, Jeffrey R., Lee, Michael S., Rossi, Cynthia A., McCarthy, Sarah E., Radoshitzky, Sheli R., Dye, John M., Hensley, Lisa E., Honko, Anna, Kuhn, Jens H., Jahrling, Peter B., Warren, Travis K., Whitehouse, Chris A., Bavari, Sina, Palacios, Gustavo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3509072/
https://www.ncbi.nlm.nih.gov/pubmed/23209706
http://dx.doi.org/10.1371/journal.pone.0050316
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author Kugelman, Jeffrey R.
Lee, Michael S.
Rossi, Cynthia A.
McCarthy, Sarah E.
Radoshitzky, Sheli R.
Dye, John M.
Hensley, Lisa E.
Honko, Anna
Kuhn, Jens H.
Jahrling, Peter B.
Warren, Travis K.
Whitehouse, Chris A.
Bavari, Sina
Palacios, Gustavo
author_facet Kugelman, Jeffrey R.
Lee, Michael S.
Rossi, Cynthia A.
McCarthy, Sarah E.
Radoshitzky, Sheli R.
Dye, John M.
Hensley, Lisa E.
Honko, Anna
Kuhn, Jens H.
Jahrling, Peter B.
Warren, Travis K.
Whitehouse, Chris A.
Bavari, Sina
Palacios, Gustavo
author_sort Kugelman, Jeffrey R.
collection PubMed
description To identify polymorphic sites that could be used as biomarkers of Ebola virus passage history, we repeatedly amplified Ebola virus (Kikwit variant) in vitro and in vivo and performed deep sequencing analysis of the complete genomes of the viral subpopulations. We then determined the sites undergoing selection during passage in Vero E6 cells. Four locations within the Ebola virus Kikwit genome were identified that together segregate cell culture-passaged virus and virus obtained from infected non-human primates. Three of the identified sites are located within the glycoprotein gene (GP) sequence: the poly-U (RNA editing) site at position 6925, as well as positions 6677, and 6179. One site was found in the VP24 gene at position 10833. In all cases, in vitro and in vivo, both populations (majority and minority variants) were maintained in the viral swarm, with rapid selections occurring after a few passages or infections. This analysis approach will be useful to differentiate whether filovirus stocks with unknown history have been passaged in cell culture and may support filovirus stock standardization for medical countermeasure development.
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spelling pubmed-35090722012-12-03 Ebola Virus Genome Plasticity as a Marker of Its Passaging History: A Comparison of In Vitro Passaging to Non-Human Primate Infection Kugelman, Jeffrey R. Lee, Michael S. Rossi, Cynthia A. McCarthy, Sarah E. Radoshitzky, Sheli R. Dye, John M. Hensley, Lisa E. Honko, Anna Kuhn, Jens H. Jahrling, Peter B. Warren, Travis K. Whitehouse, Chris A. Bavari, Sina Palacios, Gustavo PLoS One Research Article To identify polymorphic sites that could be used as biomarkers of Ebola virus passage history, we repeatedly amplified Ebola virus (Kikwit variant) in vitro and in vivo and performed deep sequencing analysis of the complete genomes of the viral subpopulations. We then determined the sites undergoing selection during passage in Vero E6 cells. Four locations within the Ebola virus Kikwit genome were identified that together segregate cell culture-passaged virus and virus obtained from infected non-human primates. Three of the identified sites are located within the glycoprotein gene (GP) sequence: the poly-U (RNA editing) site at position 6925, as well as positions 6677, and 6179. One site was found in the VP24 gene at position 10833. In all cases, in vitro and in vivo, both populations (majority and minority variants) were maintained in the viral swarm, with rapid selections occurring after a few passages or infections. This analysis approach will be useful to differentiate whether filovirus stocks with unknown history have been passaged in cell culture and may support filovirus stock standardization for medical countermeasure development. Public Library of Science 2012-11-28 /pmc/articles/PMC3509072/ /pubmed/23209706 http://dx.doi.org/10.1371/journal.pone.0050316 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration, which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose.
spellingShingle Research Article
Kugelman, Jeffrey R.
Lee, Michael S.
Rossi, Cynthia A.
McCarthy, Sarah E.
Radoshitzky, Sheli R.
Dye, John M.
Hensley, Lisa E.
Honko, Anna
Kuhn, Jens H.
Jahrling, Peter B.
Warren, Travis K.
Whitehouse, Chris A.
Bavari, Sina
Palacios, Gustavo
Ebola Virus Genome Plasticity as a Marker of Its Passaging History: A Comparison of In Vitro Passaging to Non-Human Primate Infection
title Ebola Virus Genome Plasticity as a Marker of Its Passaging History: A Comparison of In Vitro Passaging to Non-Human Primate Infection
title_full Ebola Virus Genome Plasticity as a Marker of Its Passaging History: A Comparison of In Vitro Passaging to Non-Human Primate Infection
title_fullStr Ebola Virus Genome Plasticity as a Marker of Its Passaging History: A Comparison of In Vitro Passaging to Non-Human Primate Infection
title_full_unstemmed Ebola Virus Genome Plasticity as a Marker of Its Passaging History: A Comparison of In Vitro Passaging to Non-Human Primate Infection
title_short Ebola Virus Genome Plasticity as a Marker of Its Passaging History: A Comparison of In Vitro Passaging to Non-Human Primate Infection
title_sort ebola virus genome plasticity as a marker of its passaging history: a comparison of in vitro passaging to non-human primate infection
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3509072/
https://www.ncbi.nlm.nih.gov/pubmed/23209706
http://dx.doi.org/10.1371/journal.pone.0050316
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