Genome Evolution of Two Genetically Homogeneous Infectious Bursal Disease Virus Strains During Passages in vitro and ex vivo in the Presence of a Mutagenic Nucleoside Analog

The avibirnavirus infectious bursal disease virus (IBDV) is responsible for a highly contagious and sometimes lethal disease of chickens (Gallus gallus). IBDV genetic variation is well-described for both field and live-attenuated vaccine strains, however, the dynamics and selection pressures behind...

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Autores principales: Cubas-Gaona, Liliana L., Flageul, Alexandre, Courtillon, Céline, Briand, Francois-Xavier, Contrant, Maud, Bougeard, Stephanie, Lucas, Pierrick, Quenault, Hélène, Leroux, Aurélie, Keita, Alassane, Amelot, Michel, Grasland, Béatrice, Blanchard, Yannick, Eterradossi, Nicolas, Brown, Paul Alun, Soubies, Sébastien Mathieu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8226269/
https://www.ncbi.nlm.nih.gov/pubmed/34177862
http://dx.doi.org/10.3389/fmicb.2021.678563
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author Cubas-Gaona, Liliana L.
Flageul, Alexandre
Courtillon, Céline
Briand, Francois-Xavier
Contrant, Maud
Bougeard, Stephanie
Lucas, Pierrick
Quenault, Hélène
Leroux, Aurélie
Keita, Alassane
Amelot, Michel
Grasland, Béatrice
Blanchard, Yannick
Eterradossi, Nicolas
Brown, Paul Alun
Soubies, Sébastien Mathieu
author_facet Cubas-Gaona, Liliana L.
Flageul, Alexandre
Courtillon, Céline
Briand, Francois-Xavier
Contrant, Maud
Bougeard, Stephanie
Lucas, Pierrick
Quenault, Hélène
Leroux, Aurélie
Keita, Alassane
Amelot, Michel
Grasland, Béatrice
Blanchard, Yannick
Eterradossi, Nicolas
Brown, Paul Alun
Soubies, Sébastien Mathieu
author_sort Cubas-Gaona, Liliana L.
collection PubMed
description The avibirnavirus infectious bursal disease virus (IBDV) is responsible for a highly contagious and sometimes lethal disease of chickens (Gallus gallus). IBDV genetic variation is well-described for both field and live-attenuated vaccine strains, however, the dynamics and selection pressures behind this genetic evolution remain poorly documented. Here, genetically homogeneous virus stocks were generated using reverse genetics for a very virulent strain, rvv, and a vaccine-related strain, rCu-1. These viruses were serially passaged at controlled multiplicities of infection in several biological systems, including primary chickens B cells, the main cell type targeted by IBDV in vivo. Passages were also performed in the absence or presence of a strong selective pressure using the antiviral nucleoside analog 7-deaza-2′-C-methyladenosine (7DMA). Next Generation Sequencing (NGS) of viral genomes after the last passage in each biological system revealed that (i) a higher viral diversity was generated in segment A than in segment B, regardless 7DMA treatment and viral strain, (ii) diversity in segment B was increased by 7DMA treatment in both viruses, (iii) passaging of IBDV in primary chicken B cells, regardless of 7DMA treatment, did not select cell-culture adapted variants of rvv, preserving its capsid protein (VP2) properties, (iv) mutations in coding and non-coding regions of rCu-1 segment A could potentially associate to higher viral fitness, and (v) a specific selection, upon 7DMA addition, of a Thr329Ala substitution occurred in the viral polymerase VP1. The latter change, together with Ala270Thr change in VP2, proved to be associated with viral attenuation in vivo. These results identify genome sequences that are important for IBDV evolution in response to selection pressures. Such information will help tailor better strategies for controlling IBDV infection in chickens.
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spelling pubmed-82262692021-06-26 Genome Evolution of Two Genetically Homogeneous Infectious Bursal Disease Virus Strains During Passages in vitro and ex vivo in the Presence of a Mutagenic Nucleoside Analog Cubas-Gaona, Liliana L. Flageul, Alexandre Courtillon, Céline Briand, Francois-Xavier Contrant, Maud Bougeard, Stephanie Lucas, Pierrick Quenault, Hélène Leroux, Aurélie Keita, Alassane Amelot, Michel Grasland, Béatrice Blanchard, Yannick Eterradossi, Nicolas Brown, Paul Alun Soubies, Sébastien Mathieu Front Microbiol Microbiology The avibirnavirus infectious bursal disease virus (IBDV) is responsible for a highly contagious and sometimes lethal disease of chickens (Gallus gallus). IBDV genetic variation is well-described for both field and live-attenuated vaccine strains, however, the dynamics and selection pressures behind this genetic evolution remain poorly documented. Here, genetically homogeneous virus stocks were generated using reverse genetics for a very virulent strain, rvv, and a vaccine-related strain, rCu-1. These viruses were serially passaged at controlled multiplicities of infection in several biological systems, including primary chickens B cells, the main cell type targeted by IBDV in vivo. Passages were also performed in the absence or presence of a strong selective pressure using the antiviral nucleoside analog 7-deaza-2′-C-methyladenosine (7DMA). Next Generation Sequencing (NGS) of viral genomes after the last passage in each biological system revealed that (i) a higher viral diversity was generated in segment A than in segment B, regardless 7DMA treatment and viral strain, (ii) diversity in segment B was increased by 7DMA treatment in both viruses, (iii) passaging of IBDV in primary chicken B cells, regardless of 7DMA treatment, did not select cell-culture adapted variants of rvv, preserving its capsid protein (VP2) properties, (iv) mutations in coding and non-coding regions of rCu-1 segment A could potentially associate to higher viral fitness, and (v) a specific selection, upon 7DMA addition, of a Thr329Ala substitution occurred in the viral polymerase VP1. The latter change, together with Ala270Thr change in VP2, proved to be associated with viral attenuation in vivo. These results identify genome sequences that are important for IBDV evolution in response to selection pressures. Such information will help tailor better strategies for controlling IBDV infection in chickens. Frontiers Media S.A. 2021-06-11 /pmc/articles/PMC8226269/ /pubmed/34177862 http://dx.doi.org/10.3389/fmicb.2021.678563 Text en Copyright © 2021 Cubas-Gaona, Flageul, Courtillon, Briand, Contrant, Bougeard, Lucas, Quenault, Leroux, Keita, Amelot, Grasland, Blanchard, Eterradossi, Brown and Soubies. https://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
Cubas-Gaona, Liliana L.
Flageul, Alexandre
Courtillon, Céline
Briand, Francois-Xavier
Contrant, Maud
Bougeard, Stephanie
Lucas, Pierrick
Quenault, Hélène
Leroux, Aurélie
Keita, Alassane
Amelot, Michel
Grasland, Béatrice
Blanchard, Yannick
Eterradossi, Nicolas
Brown, Paul Alun
Soubies, Sébastien Mathieu
Genome Evolution of Two Genetically Homogeneous Infectious Bursal Disease Virus Strains During Passages in vitro and ex vivo in the Presence of a Mutagenic Nucleoside Analog
title Genome Evolution of Two Genetically Homogeneous Infectious Bursal Disease Virus Strains During Passages in vitro and ex vivo in the Presence of a Mutagenic Nucleoside Analog
title_full Genome Evolution of Two Genetically Homogeneous Infectious Bursal Disease Virus Strains During Passages in vitro and ex vivo in the Presence of a Mutagenic Nucleoside Analog
title_fullStr Genome Evolution of Two Genetically Homogeneous Infectious Bursal Disease Virus Strains During Passages in vitro and ex vivo in the Presence of a Mutagenic Nucleoside Analog
title_full_unstemmed Genome Evolution of Two Genetically Homogeneous Infectious Bursal Disease Virus Strains During Passages in vitro and ex vivo in the Presence of a Mutagenic Nucleoside Analog
title_short Genome Evolution of Two Genetically Homogeneous Infectious Bursal Disease Virus Strains During Passages in vitro and ex vivo in the Presence of a Mutagenic Nucleoside Analog
title_sort genome evolution of two genetically homogeneous infectious bursal disease virus strains during passages in vitro and ex vivo in the presence of a mutagenic nucleoside analog
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8226269/
https://www.ncbi.nlm.nih.gov/pubmed/34177862
http://dx.doi.org/10.3389/fmicb.2021.678563
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