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The B1.351 and P.1 variants extend SARS-CoV-2 host range to mice
Xavier Montagutelli; Matthieu Prot; Laurine Levillayer; Eduard Baquero Salazar; Gregory Jouvion; Laurine Conquet; Maxima Beretta; Flora Donati; Melanie Albert; Fabiana Gambaro; Sylvie Behillil; Vincent Enouf; Dominique Rousset; Jean Jaubert; Sylvie van der Werf; Hugo Mouquet; Felix Rey; Etienne Simon-Loriere.
Affiliation
  • Xavier Montagutelli; Institut Pasteur
  • Matthieu Prot; Institut Pasteur
  • Laurine Levillayer; Institut Pasteur
  • Eduard Baquero Salazar; Institut Pasteur
  • Gregory Jouvion; Ecole Nationale Veterinaire
  • Laurine Conquet; Institut Pasteur
  • Maxima Beretta; Institut Pasteur
  • Flora Donati; Institut Pasteur
  • Melanie Albert; Institut Pasteur
  • Fabiana Gambaro; Institut Pasteur
  • Sylvie Behillil; Institut Pasteur
  • Vincent Enouf; Institut Pasteur
  • Dominique Rousset; Institut Pasteur de la Guyane
  • Jean Jaubert; Institut Pasteur
  • Sylvie van der Werf; Institut Pasteur
  • Hugo Mouquet; Institut Pasteur
  • Felix Rey; Institut Pasteur
  • Etienne Simon-Loriere; Institut Pasteur
Preprint in English | bioRxiv | ID: ppbiorxiv-436013
ABSTRACT
Receptor recognition is a major determinant of viral host range, infectivity and pathogenesis. Emergences have been associated with serendipitous events of adaptation upon encounters with novel hosts, and the high mutation rate of RNA viruses may explain their frequent host shifts. SARS-CoV-2 extensive circulation in humans results in the emergence of variants, including variants of concern (VOCs) with diverse mutations notably in the spike, and increased transmissibility or immune escape. Here we show that, unlike the initial and Delta variants, the three VOCs bearing the N501Y mutation can infect common laboratory mice. Contact transmission occurred from infected to naive mice through two passages. This host range expansion likely results from an increased binding of the spike to the mouse ACE2. Together with the observed contact transmission, it raises the possibility of wild rodent secondary reservoirs enabling the emergence of new variants.
License
cc_by_nc_nd
Full text: Available Collection: Preprints Database: bioRxiv Language: English Year: 2021 Document type: Preprint
Full text: Available Collection: Preprints Database: bioRxiv Language: English Year: 2021 Document type: Preprint
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