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The B.1.427/1.429 (epsilon) SARS-CoV-2 variants are more virulent than ancestral B.1 (614G) in Syrian hamsters

As novel SARS-CoV-2 variants continue to emerge, it is critical that their potential to cause severe disease and evade vaccine-induced immunity is rapidly assessed in humans and studied in animal models. In early January 2021, a novel variant of concern (VOC) designated B.1.429 comprising 2 lineages...

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Autores principales: Carroll, Timothy, Fox, Douglas, van Doremalen, Neeltje, Ball, Erin, Morris, Mary Kate, Sotomayor-Gonzalez, Alicia, Servellita, Venice, Rustagi, Arjun, Yinda, Claude Kwe, Fritts, Linda, Port, Julia Rebecca, Ma, Zhong-Min, Holbrook, Myndi, Schulz, Jonathan, Blish, Catherine A., Hanson, Carl, Chiu, Charles Y., Munster, Vincent, Stanley, Sarah, Miller, Christopher J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8404898/
https://www.ncbi.nlm.nih.gov/pubmed/34462750
http://dx.doi.org/10.1101/2021.08.25.457626
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author Carroll, Timothy
Fox, Douglas
van Doremalen, Neeltje
Ball, Erin
Morris, Mary Kate
Sotomayor-Gonzalez, Alicia
Servellita, Venice
Rustagi, Arjun
Yinda, Claude Kwe
Fritts, Linda
Port, Julia Rebecca
Ma, Zhong-Min
Holbrook, Myndi
Schulz, Jonathan
Blish, Catherine A.
Hanson, Carl
Chiu, Charles Y.
Munster, Vincent
Stanley, Sarah
Miller, Christopher J.
author_facet Carroll, Timothy
Fox, Douglas
van Doremalen, Neeltje
Ball, Erin
Morris, Mary Kate
Sotomayor-Gonzalez, Alicia
Servellita, Venice
Rustagi, Arjun
Yinda, Claude Kwe
Fritts, Linda
Port, Julia Rebecca
Ma, Zhong-Min
Holbrook, Myndi
Schulz, Jonathan
Blish, Catherine A.
Hanson, Carl
Chiu, Charles Y.
Munster, Vincent
Stanley, Sarah
Miller, Christopher J.
author_sort Carroll, Timothy
collection PubMed
description As novel SARS-CoV-2 variants continue to emerge, it is critical that their potential to cause severe disease and evade vaccine-induced immunity is rapidly assessed in humans and studied in animal models. In early January 2021, a novel variant of concern (VOC) designated B.1.429 comprising 2 lineages, B.1.427 and B.1.429, was originally detected in California (CA) and shown to enhance infectivity in vitro and decrease antibody neutralization by plasma from convalescent patients and vaccine recipients. Here we examine the virulence, transmissibility, and susceptibility to pre-existing immunity for B 1.427 and B 1.429 in the Syrian hamster model. We find that both strains exhibit enhanced virulence as measured by increased body weight loss compared to hamsters infected with ancestral B.1 (614G), with B.1.429 causing the most body weight loss among all 3 lineages. Faster dissemination from airways to parenchyma and more severe lung pathology at both early and late stages were also observed with B.1.429 infections relative to B.1. (614G) and B.1.427 infections. In addition, subgenomic viral RNA (sgRNA) levels were highest in oral swabs of hamsters infected with B.1.429, however sgRNA levels in lungs were similar in all three strains. This demonstrates that B.1.429 replicates to higher levels than ancestral B.1 (614G) or B.1.427 in the upper respiratory tract (URT) but not in the lungs. In multi-virus in-vivo competition experiments, we found that epsilon (B.1.427/B.1.429) and gamma (P.1) dramatically outcompete alpha (B.1.1.7), beta (B.1.351) and zeta (P.2) in the lungs. In the URT gamma, and epsilon dominate, but the highly infectious alpha variant also maintains a moderate size niche. We did not observe significant differences in airborne transmission efficiency among the B.1.427, B.1.429 and ancestral B.1 (614G) variants in hamsters. These results demonstrate enhanced virulence and high relative fitness of the epsilon (B.1.427/B.1.429) variant in Syrian hamsters compared to an ancestral B.1 (614G) strain.
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spelling pubmed-84048982021-08-31 The B.1.427/1.429 (epsilon) SARS-CoV-2 variants are more virulent than ancestral B.1 (614G) in Syrian hamsters Carroll, Timothy Fox, Douglas van Doremalen, Neeltje Ball, Erin Morris, Mary Kate Sotomayor-Gonzalez, Alicia Servellita, Venice Rustagi, Arjun Yinda, Claude Kwe Fritts, Linda Port, Julia Rebecca Ma, Zhong-Min Holbrook, Myndi Schulz, Jonathan Blish, Catherine A. Hanson, Carl Chiu, Charles Y. Munster, Vincent Stanley, Sarah Miller, Christopher J. bioRxiv Article As novel SARS-CoV-2 variants continue to emerge, it is critical that their potential to cause severe disease and evade vaccine-induced immunity is rapidly assessed in humans and studied in animal models. In early January 2021, a novel variant of concern (VOC) designated B.1.429 comprising 2 lineages, B.1.427 and B.1.429, was originally detected in California (CA) and shown to enhance infectivity in vitro and decrease antibody neutralization by plasma from convalescent patients and vaccine recipients. Here we examine the virulence, transmissibility, and susceptibility to pre-existing immunity for B 1.427 and B 1.429 in the Syrian hamster model. We find that both strains exhibit enhanced virulence as measured by increased body weight loss compared to hamsters infected with ancestral B.1 (614G), with B.1.429 causing the most body weight loss among all 3 lineages. Faster dissemination from airways to parenchyma and more severe lung pathology at both early and late stages were also observed with B.1.429 infections relative to B.1. (614G) and B.1.427 infections. In addition, subgenomic viral RNA (sgRNA) levels were highest in oral swabs of hamsters infected with B.1.429, however sgRNA levels in lungs were similar in all three strains. This demonstrates that B.1.429 replicates to higher levels than ancestral B.1 (614G) or B.1.427 in the upper respiratory tract (URT) but not in the lungs. In multi-virus in-vivo competition experiments, we found that epsilon (B.1.427/B.1.429) and gamma (P.1) dramatically outcompete alpha (B.1.1.7), beta (B.1.351) and zeta (P.2) in the lungs. In the URT gamma, and epsilon dominate, but the highly infectious alpha variant also maintains a moderate size niche. We did not observe significant differences in airborne transmission efficiency among the B.1.427, B.1.429 and ancestral B.1 (614G) variants in hamsters. These results demonstrate enhanced virulence and high relative fitness of the epsilon (B.1.427/B.1.429) variant in Syrian hamsters compared to an ancestral B.1 (614G) strain. Cold Spring Harbor Laboratory 2021-08-25 /pmc/articles/PMC8404898/ /pubmed/34462750 http://dx.doi.org/10.1101/2021.08.25.457626 Text en https://creativecommons.org/publicdomain/zero/1.0/This article is a US Government work. It is not subject to copyright under 17 USC 105 and is also made available for use under a CC0 license (https://creativecommons.org/publicdomain/zero/1.0/) .
spellingShingle Article
Carroll, Timothy
Fox, Douglas
van Doremalen, Neeltje
Ball, Erin
Morris, Mary Kate
Sotomayor-Gonzalez, Alicia
Servellita, Venice
Rustagi, Arjun
Yinda, Claude Kwe
Fritts, Linda
Port, Julia Rebecca
Ma, Zhong-Min
Holbrook, Myndi
Schulz, Jonathan
Blish, Catherine A.
Hanson, Carl
Chiu, Charles Y.
Munster, Vincent
Stanley, Sarah
Miller, Christopher J.
The B.1.427/1.429 (epsilon) SARS-CoV-2 variants are more virulent than ancestral B.1 (614G) in Syrian hamsters
title The B.1.427/1.429 (epsilon) SARS-CoV-2 variants are more virulent than ancestral B.1 (614G) in Syrian hamsters
title_full The B.1.427/1.429 (epsilon) SARS-CoV-2 variants are more virulent than ancestral B.1 (614G) in Syrian hamsters
title_fullStr The B.1.427/1.429 (epsilon) SARS-CoV-2 variants are more virulent than ancestral B.1 (614G) in Syrian hamsters
title_full_unstemmed The B.1.427/1.429 (epsilon) SARS-CoV-2 variants are more virulent than ancestral B.1 (614G) in Syrian hamsters
title_short The B.1.427/1.429 (epsilon) SARS-CoV-2 variants are more virulent than ancestral B.1 (614G) in Syrian hamsters
title_sort b.1.427/1.429 (epsilon) sars-cov-2 variants are more virulent than ancestral b.1 (614g) in syrian hamsters
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8404898/
https://www.ncbi.nlm.nih.gov/pubmed/34462750
http://dx.doi.org/10.1101/2021.08.25.457626
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