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Hepatitis E Virus Shows More Genomic Alterations in Cell Culture than In Vivo

Hepatitis E Virus (HEV) mutations following ribavirin treatment have been associated with treatment non-response and viral persistence, but spontaneous occurring genomic variations have been less well characterized. We here set out to study the HEV genome composition in 2 patient sample types and 2...

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Autores principales: Sari, Gulce, van de Garde, Martijn D.B., van Schoonhoven, Anne, Voermans, Jolanda J.C., van der Eijk, Annemiek A., de Man, Robert A., Boonstra, Andre, Vanwolleghem, Thomas, Pas, Suzan D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6963849/
https://www.ncbi.nlm.nih.gov/pubmed/31766624
http://dx.doi.org/10.3390/pathogens8040255
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author Sari, Gulce
van de Garde, Martijn D.B.
van Schoonhoven, Anne
Voermans, Jolanda J.C.
van der Eijk, Annemiek A.
de Man, Robert A.
Boonstra, Andre
Vanwolleghem, Thomas
Pas, Suzan D.
author_facet Sari, Gulce
van de Garde, Martijn D.B.
van Schoonhoven, Anne
Voermans, Jolanda J.C.
van der Eijk, Annemiek A.
de Man, Robert A.
Boonstra, Andre
Vanwolleghem, Thomas
Pas, Suzan D.
author_sort Sari, Gulce
collection PubMed
description Hepatitis E Virus (HEV) mutations following ribavirin treatment have been associated with treatment non-response and viral persistence, but spontaneous occurring genomic variations have been less well characterized. We here set out to study the HEV genome composition in 2 patient sample types and 2 infection models. Near full HEV genome Sanger sequences of serum- and feces-derived HEV from two chronic HEV genotype 3 (gt3) patients were obtained. In addition, viruses were sequenced after in vitro or in vivo expansion on A549 cells or a humanized mouse model, respectively. We show that HEV acquired 19 nucleotide mutations, of which 7 nonsynonymous amino acids changes located in Open Reading Frame 1 (ORF1), ORF2, and ORF3 coding regions, after prolonged in vitro culture. In vivo passage resulted in selection of 8 nucleotide mutations with 2 altered amino acids in the X domain and Poly-proline region of ORF1. Intra-patient comparison of feces- and serum-derived HEV gt3 of two patients showed 7 and 2 nucleotide mutations with 2 and 0 amino acid changes, respectively. Overall, the number of genomic alterations was up to 1.25× per 1000 nucleotides or amino acids in in vivo samples, and up to 2.84× after in vitro expansion of the same clinical HEV strain. In vitro replication of a clinical HEV strain is therefore associated with more mutations, compared to the minor HEV genomic alterations seen after passage of the same strain in an immune deficient humanized mouse; as well as in feces and blood of 2 immunosuppressed chronically infected HEV patients. These data suggest that HEV infected humanized mice more closely reflect the HEV biology seen in solid organ transplant recipients.
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spelling pubmed-69638492020-01-27 Hepatitis E Virus Shows More Genomic Alterations in Cell Culture than In Vivo Sari, Gulce van de Garde, Martijn D.B. van Schoonhoven, Anne Voermans, Jolanda J.C. van der Eijk, Annemiek A. de Man, Robert A. Boonstra, Andre Vanwolleghem, Thomas Pas, Suzan D. Pathogens Article Hepatitis E Virus (HEV) mutations following ribavirin treatment have been associated with treatment non-response and viral persistence, but spontaneous occurring genomic variations have been less well characterized. We here set out to study the HEV genome composition in 2 patient sample types and 2 infection models. Near full HEV genome Sanger sequences of serum- and feces-derived HEV from two chronic HEV genotype 3 (gt3) patients were obtained. In addition, viruses were sequenced after in vitro or in vivo expansion on A549 cells or a humanized mouse model, respectively. We show that HEV acquired 19 nucleotide mutations, of which 7 nonsynonymous amino acids changes located in Open Reading Frame 1 (ORF1), ORF2, and ORF3 coding regions, after prolonged in vitro culture. In vivo passage resulted in selection of 8 nucleotide mutations with 2 altered amino acids in the X domain and Poly-proline region of ORF1. Intra-patient comparison of feces- and serum-derived HEV gt3 of two patients showed 7 and 2 nucleotide mutations with 2 and 0 amino acid changes, respectively. Overall, the number of genomic alterations was up to 1.25× per 1000 nucleotides or amino acids in in vivo samples, and up to 2.84× after in vitro expansion of the same clinical HEV strain. In vitro replication of a clinical HEV strain is therefore associated with more mutations, compared to the minor HEV genomic alterations seen after passage of the same strain in an immune deficient humanized mouse; as well as in feces and blood of 2 immunosuppressed chronically infected HEV patients. These data suggest that HEV infected humanized mice more closely reflect the HEV biology seen in solid organ transplant recipients. MDPI 2019-11-22 /pmc/articles/PMC6963849/ /pubmed/31766624 http://dx.doi.org/10.3390/pathogens8040255 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
Sari, Gulce
van de Garde, Martijn D.B.
van Schoonhoven, Anne
Voermans, Jolanda J.C.
van der Eijk, Annemiek A.
de Man, Robert A.
Boonstra, Andre
Vanwolleghem, Thomas
Pas, Suzan D.
Hepatitis E Virus Shows More Genomic Alterations in Cell Culture than In Vivo
title Hepatitis E Virus Shows More Genomic Alterations in Cell Culture than In Vivo
title_full Hepatitis E Virus Shows More Genomic Alterations in Cell Culture than In Vivo
title_fullStr Hepatitis E Virus Shows More Genomic Alterations in Cell Culture than In Vivo
title_full_unstemmed Hepatitis E Virus Shows More Genomic Alterations in Cell Culture than In Vivo
title_short Hepatitis E Virus Shows More Genomic Alterations in Cell Culture than In Vivo
title_sort hepatitis e virus shows more genomic alterations in cell culture than in vivo
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6963849/
https://www.ncbi.nlm.nih.gov/pubmed/31766624
http://dx.doi.org/10.3390/pathogens8040255
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