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  3. Enhanced fitness of SARS-CoV-2 variant of concern Alpha but not Beta.
 

Enhanced fitness of SARS-CoV-2 variant of concern Alpha but not Beta.

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BORIS DOI
10.48350/163848
Date of Publication
February 2022
Publication Type
Article
Division/Institute

Institut für Virologi...

Institut für Veterinä...

Institut für Infektio...

Department of Infecti...

Institut für Infektio...

Author
Ulrich, Lorenz
Halwe, Nico Joel
Taddeo, Adrianoorcid-logo
Institut für Virologie und Immunologie (IVI)
Ebert, Nadine
Department of Infectious Diseases and Pathobiology (DIP)
Schön, Jacob
Devisme, Christelle
Institut für Virologie und Immunologie (IVI)
Trüeb, Bettina Salome
Institut für Veterinärbakteriologie (IVB)
Hoffmann, Bernd
Licheri, Manon Flore
Institut für Infektionskrankheiten, Forschung
Fan, Xiaoyu
Bekliz, Meriem
Essaidi-Laziosi, Manel
Schmidt, Marie Luisa
Niemeyer, Daniela
Corman, Victor Max
Kraft, Anna
Godel, Aurélie
Institut für Virologie und Immunologie (IVI)
Laloli, Laura
Institut für Infektionskrankheiten, Forschung
Kelly, Jenna Nicole
Institut für Virologie und Immunologie (IVI)
Calderon, Brenda M
Breithaupt, Angele
Wylezich, Claudia
Veiga, Inês Berenguer
Gultom, Mitra Lovelin
Institut für Infektionskrankheiten, Forschung
Osman, Sarah
Zhou, Bin
Adea, Kenneth
Meyer, Benjamin
Eberhardt, Christiane
Thomann, Lisa Jane
Institut für Virologie und Immunologie (IVI)
Gsell-Albert, Monika
Institut für Infektionskrankheiten (IFIK)
Labroussaa, Fabien
Institut für Veterinärbakteriologie (IVB)
Jores, Jörgorcid-logo
Institut für Veterinärbakteriologie (IVB)
Summerfield, Arturorcid-logo
Institut für Virologie und Immunologie (IVI)
Drosten, Christian
Eckerle, Isabella Anne
Wentworth, David E
Dijkman, Ronaldorcid-logo
Institut für Infektionskrankheiten (IFIK)
Institut für Infektionskrankheiten, Forschung
Hoffmann, Donata
Thiel, Volker Earl
Department of Infectious Diseases and Pathobiology (DIP)
Beer, Martin
Benarafa, Charaforcid-logo
Institut für Virologie und Immunologie (IVI)
Subject(s)

500 - Science::570 - ...

600 - Technology::610...

600 - Technology::630...

Series
Nature
ISSN or ISBN (if monograph)
1476-4687
Publisher
Springer Nature
Language
English
Publisher DOI
10.1038/s41586-021-04342-0
PubMed ID
34937050
Description
Emerging variants of concern (VOC) drive the SARS-CoV-2 pandemic1,2. Experimental assessment of replication and transmission of major VOC compared to progenitors are needed to understand successful emerging mechanisms of VOC3. Here, we show that Alpha and Beta spike (S) proteins have a greater affinity to human angiotensin converting enzyme 2 (hACE2) receptor over the progenitor variant (wt-S614G) in vitro. Yet Alpha and wt-S614G had similar replication kinetics in human nasal airway epithelial cultures, whereas Beta was outcompeted by both. In vivo, competition experiments showed a clear fitness advantage of Alpha over the progenitor variant (wt-S614G) in ferrets and two mouse models, where the substitutions in S were major drivers for fitness advantage. In hamsters, supporting high replication levels, Alpha and wt-S614G had comparable fitness. In contrast, Beta was outcompeted by Alpha and wt-S614G in hamsters and hACE2-expressing mice. Our study highlights the importance of using multiple models for complete fitness characterization of VOC and demonstrates adaptation of Alpha towards increased upper respiratory tract replication and enhanced transmission in vivo in restrictive models, whereas Beta fails to overcome contemporary strains in naïve animals.
Handle
https://boris-portal.unibe.ch/handle/20.500.12422/59554
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s41586-021-04342-0_reference.pdftextAdobe PDF17.83 MBacceptedOpen
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