Andes Virus Genome Mutations That Are Likely Associated with Animal Model Attenuation and Human Person-to-Person Transmission

We performed whole-genome sequencing with bait enrichment techniques to analyze Andes virus (ANDV), a cause of human hantavirus pulmonary syndrome. We used cryopreserved lung tissues from a naturally infected long-tailed colilargo, including early, intermediate, and late cell culture, passages of an...

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Autores principales: Bellomo, Carla M., Alonso, Daniel O., Pérez-Sautu, Unai, Prieto, Karla, Kehl, Sebastian, Coelho, Rocio M., Periolo, Natalia, Di Paola, Nicholas, Ferressini-Gerpe, Natalia, Kuhn, Jens H., Sanchez-Lockhart, Mariano, Palacios, Gustavo, Martínez, Valeria P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10286707/
https://www.ncbi.nlm.nih.gov/pubmed/37097182
http://dx.doi.org/10.1128/msphere.00018-23
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author Bellomo, Carla M.
Alonso, Daniel O.
Pérez-Sautu, Unai
Prieto, Karla
Kehl, Sebastian
Coelho, Rocio M.
Periolo, Natalia
Di Paola, Nicholas
Ferressini-Gerpe, Natalia
Kuhn, Jens H.
Sanchez-Lockhart, Mariano
Palacios, Gustavo
Martínez, Valeria P.
author_facet Bellomo, Carla M.
Alonso, Daniel O.
Pérez-Sautu, Unai
Prieto, Karla
Kehl, Sebastian
Coelho, Rocio M.
Periolo, Natalia
Di Paola, Nicholas
Ferressini-Gerpe, Natalia
Kuhn, Jens H.
Sanchez-Lockhart, Mariano
Palacios, Gustavo
Martínez, Valeria P.
author_sort Bellomo, Carla M.
collection PubMed
description We performed whole-genome sequencing with bait enrichment techniques to analyze Andes virus (ANDV), a cause of human hantavirus pulmonary syndrome. We used cryopreserved lung tissues from a naturally infected long-tailed colilargo, including early, intermediate, and late cell culture, passages of an ANDV isolate from that animal, and lung tissues from golden hamsters experimentally exposed to that ANDV isolate. The resulting complete genome sequences were subjected to detailed comparative genomic analysis against American orthohantaviruses. We identified four amino acid substitutions related to cell culture adaptation that resulted in attenuation of ANDV in the typically lethal golden hamster animal model of hantavirus pulmonary syndrome. Changes in the ANDV nucleocapsid protein, glycoprotein, and small nonstructural protein open reading frames correlated with mutations typical for ANDV strains associated with increased virulence in the small-animal model. Finally, we identified three amino acid substitutions, two in the small nonstructural protein and one in the glycoprotein, that were only present in the clade of viruses associated with efficient person-to-person transmission. Our results indicate that there are single-nucleotide polymorphisms that could be used to predict strain-specific ANDV virulence and/or transmissibility. IMPORTANCE Several orthohantaviruses cause the zoonotic disease hantavirus pulmonary syndrome (HPS) in the Americas. Among them, HPS caused by Andes virus (ANDV) is of great public health concern because it is associated with the highest case fatality rate (up to 50%). ANDV is also the only orthohantavirus associated with relatively robust evidence of person-to-person transmission. This work reveals nucleotide changes in the ANDV genome that are associated with virulence attenuation in an animal model and increased transmissibility in humans. These findings may pave the way to early severity predictions in future ANDV-caused HPS outbreaks.
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spelling pubmed-102867072023-06-23 Andes Virus Genome Mutations That Are Likely Associated with Animal Model Attenuation and Human Person-to-Person Transmission Bellomo, Carla M. Alonso, Daniel O. Pérez-Sautu, Unai Prieto, Karla Kehl, Sebastian Coelho, Rocio M. Periolo, Natalia Di Paola, Nicholas Ferressini-Gerpe, Natalia Kuhn, Jens H. Sanchez-Lockhart, Mariano Palacios, Gustavo Martínez, Valeria P. mSphere Research Article We performed whole-genome sequencing with bait enrichment techniques to analyze Andes virus (ANDV), a cause of human hantavirus pulmonary syndrome. We used cryopreserved lung tissues from a naturally infected long-tailed colilargo, including early, intermediate, and late cell culture, passages of an ANDV isolate from that animal, and lung tissues from golden hamsters experimentally exposed to that ANDV isolate. The resulting complete genome sequences were subjected to detailed comparative genomic analysis against American orthohantaviruses. We identified four amino acid substitutions related to cell culture adaptation that resulted in attenuation of ANDV in the typically lethal golden hamster animal model of hantavirus pulmonary syndrome. Changes in the ANDV nucleocapsid protein, glycoprotein, and small nonstructural protein open reading frames correlated with mutations typical for ANDV strains associated with increased virulence in the small-animal model. Finally, we identified three amino acid substitutions, two in the small nonstructural protein and one in the glycoprotein, that were only present in the clade of viruses associated with efficient person-to-person transmission. Our results indicate that there are single-nucleotide polymorphisms that could be used to predict strain-specific ANDV virulence and/or transmissibility. IMPORTANCE Several orthohantaviruses cause the zoonotic disease hantavirus pulmonary syndrome (HPS) in the Americas. Among them, HPS caused by Andes virus (ANDV) is of great public health concern because it is associated with the highest case fatality rate (up to 50%). ANDV is also the only orthohantavirus associated with relatively robust evidence of person-to-person transmission. This work reveals nucleotide changes in the ANDV genome that are associated with virulence attenuation in an animal model and increased transmissibility in humans. These findings may pave the way to early severity predictions in future ANDV-caused HPS outbreaks. American Society for Microbiology 2023-04-25 /pmc/articles/PMC10286707/ /pubmed/37097182 http://dx.doi.org/10.1128/msphere.00018-23 Text en https://doi.org/10.1128/AuthorWarrantyLicense.v1This is a work of the U.S. Government and is not subject to copyright protection in the United States. Foreign copyrights may apply.
spellingShingle Research Article
Bellomo, Carla M.
Alonso, Daniel O.
Pérez-Sautu, Unai
Prieto, Karla
Kehl, Sebastian
Coelho, Rocio M.
Periolo, Natalia
Di Paola, Nicholas
Ferressini-Gerpe, Natalia
Kuhn, Jens H.
Sanchez-Lockhart, Mariano
Palacios, Gustavo
Martínez, Valeria P.
Andes Virus Genome Mutations That Are Likely Associated with Animal Model Attenuation and Human Person-to-Person Transmission
title Andes Virus Genome Mutations That Are Likely Associated with Animal Model Attenuation and Human Person-to-Person Transmission
title_full Andes Virus Genome Mutations That Are Likely Associated with Animal Model Attenuation and Human Person-to-Person Transmission
title_fullStr Andes Virus Genome Mutations That Are Likely Associated with Animal Model Attenuation and Human Person-to-Person Transmission
title_full_unstemmed Andes Virus Genome Mutations That Are Likely Associated with Animal Model Attenuation and Human Person-to-Person Transmission
title_short Andes Virus Genome Mutations That Are Likely Associated with Animal Model Attenuation and Human Person-to-Person Transmission
title_sort andes virus genome mutations that are likely associated with animal model attenuation and human person-to-person transmission
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10286707/
https://www.ncbi.nlm.nih.gov/pubmed/37097182
http://dx.doi.org/10.1128/msphere.00018-23
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