Insertions and Duplications in the Polyproline Region of the Hepatitis E Virus

Recombinant strains of hepatitis E virus (HEV) with insertions of human genomic fragments or HEV sequence duplications in the sequence encoding the polyproline region (PPR) were previously described in chronically infected patients. Such genomic rearrangements confer a replicative advantage in vitro...

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Autores principales: Lhomme, Sébastien, Nicot, Florence, Jeanne, Nicolas, Dimeglio, Chloé, Roulet, Alain, Lefebvre, Caroline, Carcenac, Romain, Manno, Maxime, Dubois, Martine, Peron, Jean-Marie, Alric, Laurent, Kamar, Nassim, Abravanel, Florence, Izopet, Jacques
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7004952/
https://www.ncbi.nlm.nih.gov/pubmed/32082274
http://dx.doi.org/10.3389/fmicb.2020.00001
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author Lhomme, Sébastien
Nicot, Florence
Jeanne, Nicolas
Dimeglio, Chloé
Roulet, Alain
Lefebvre, Caroline
Carcenac, Romain
Manno, Maxime
Dubois, Martine
Peron, Jean-Marie
Alric, Laurent
Kamar, Nassim
Abravanel, Florence
Izopet, Jacques
author_facet Lhomme, Sébastien
Nicot, Florence
Jeanne, Nicolas
Dimeglio, Chloé
Roulet, Alain
Lefebvre, Caroline
Carcenac, Romain
Manno, Maxime
Dubois, Martine
Peron, Jean-Marie
Alric, Laurent
Kamar, Nassim
Abravanel, Florence
Izopet, Jacques
author_sort Lhomme, Sébastien
collection PubMed
description Recombinant strains of hepatitis E virus (HEV) with insertions of human genomic fragments or HEV sequence duplications in the sequence encoding the polyproline region (PPR) were previously described in chronically infected patients. Such genomic rearrangements confer a replicative advantage in vitro but little is known about their frequency, location, or origin. As the sequences of only a few virus genomes are available, we analyzed the complete genomes of 114 HEV genotype 3 strains from immunocompromised (n = 85) and immunocompetent (n = 29) patients using the single molecular real-time sequencing method to determine the frequency, location, and origin of inserted genomic fragments, plus the proportions of variants with genomic rearrangements in each virus quasispecies. We also examined the amino acid compositions and post-translational modifications conferred by these rearrangements by comparing them to sequences without human gene insertions or HEV gene duplications. We found genomic rearrangements in 7/114 (6.1%) complete genome sequences (4 HEV-3f, 1 HEV-3e, 1 HEV-3 h, and 1 HEV-3chi-new), all from immunocompromised patients, and 3/7 were found at the acute phase of infection. Six of the seven patients harbored virus-host recombinant variants, including one patient with two different recombinant variants. We also detected three recombinant variants with genome duplications of the PPR or PPR + X domains in a single patient. All the genomic rearrangements (seven human fragment insertions of varying origins and three HEV genome duplications) occurred in the PPR. The sequences with genomic rearrangements had specific characteristics: increased net load (p < 0.001) and more ubiquitination (p < 0.001), phosphorylation (p < 0.001), and acetylation (p < 0.001) sites. The human fragment insertions and HEV genome duplications had slightly different characteristics. We believe this is the first description of HEV strains with genomic rearrangements in patients at the acute phase of infection; perhaps these strains are directly transmitted. Clearly, genomic rearrangements produce a greater net load with duplications and insertions having different features. Further studies are needed to clarify the mechanisms by which such modifications influence HEV replication.
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spelling pubmed-70049522020-02-20 Insertions and Duplications in the Polyproline Region of the Hepatitis E Virus Lhomme, Sébastien Nicot, Florence Jeanne, Nicolas Dimeglio, Chloé Roulet, Alain Lefebvre, Caroline Carcenac, Romain Manno, Maxime Dubois, Martine Peron, Jean-Marie Alric, Laurent Kamar, Nassim Abravanel, Florence Izopet, Jacques Front Microbiol Microbiology Recombinant strains of hepatitis E virus (HEV) with insertions of human genomic fragments or HEV sequence duplications in the sequence encoding the polyproline region (PPR) were previously described in chronically infected patients. Such genomic rearrangements confer a replicative advantage in vitro but little is known about their frequency, location, or origin. As the sequences of only a few virus genomes are available, we analyzed the complete genomes of 114 HEV genotype 3 strains from immunocompromised (n = 85) and immunocompetent (n = 29) patients using the single molecular real-time sequencing method to determine the frequency, location, and origin of inserted genomic fragments, plus the proportions of variants with genomic rearrangements in each virus quasispecies. We also examined the amino acid compositions and post-translational modifications conferred by these rearrangements by comparing them to sequences without human gene insertions or HEV gene duplications. We found genomic rearrangements in 7/114 (6.1%) complete genome sequences (4 HEV-3f, 1 HEV-3e, 1 HEV-3 h, and 1 HEV-3chi-new), all from immunocompromised patients, and 3/7 were found at the acute phase of infection. Six of the seven patients harbored virus-host recombinant variants, including one patient with two different recombinant variants. We also detected three recombinant variants with genome duplications of the PPR or PPR + X domains in a single patient. All the genomic rearrangements (seven human fragment insertions of varying origins and three HEV genome duplications) occurred in the PPR. The sequences with genomic rearrangements had specific characteristics: increased net load (p < 0.001) and more ubiquitination (p < 0.001), phosphorylation (p < 0.001), and acetylation (p < 0.001) sites. The human fragment insertions and HEV genome duplications had slightly different characteristics. We believe this is the first description of HEV strains with genomic rearrangements in patients at the acute phase of infection; perhaps these strains are directly transmitted. Clearly, genomic rearrangements produce a greater net load with duplications and insertions having different features. Further studies are needed to clarify the mechanisms by which such modifications influence HEV replication. Frontiers Media S.A. 2020-01-31 /pmc/articles/PMC7004952/ /pubmed/32082274 http://dx.doi.org/10.3389/fmicb.2020.00001 Text en Copyright © 2020 Lhomme, Nicot, Jeanne, Dimeglio, Roulet, Lefebvre, Carcenac, Manno, Dubois, Peron, Alric, Kamar, Abravanel and Izopet. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Microbiology
Lhomme, Sébastien
Nicot, Florence
Jeanne, Nicolas
Dimeglio, Chloé
Roulet, Alain
Lefebvre, Caroline
Carcenac, Romain
Manno, Maxime
Dubois, Martine
Peron, Jean-Marie
Alric, Laurent
Kamar, Nassim
Abravanel, Florence
Izopet, Jacques
Insertions and Duplications in the Polyproline Region of the Hepatitis E Virus
title Insertions and Duplications in the Polyproline Region of the Hepatitis E Virus
title_full Insertions and Duplications in the Polyproline Region of the Hepatitis E Virus
title_fullStr Insertions and Duplications in the Polyproline Region of the Hepatitis E Virus
title_full_unstemmed Insertions and Duplications in the Polyproline Region of the Hepatitis E Virus
title_short Insertions and Duplications in the Polyproline Region of the Hepatitis E Virus
title_sort insertions and duplications in the polyproline region of the hepatitis e virus
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7004952/
https://www.ncbi.nlm.nih.gov/pubmed/32082274
http://dx.doi.org/10.3389/fmicb.2020.00001
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