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The evolutionary history of ACE2 usage within the coronavirus subgenus Sarbecovirus
Heather L Wells; Michael C Letko; Gorka Lasso; Benard Ssebide; Julius Nziza; Denis K Byarugaba; Isamara Navarrete-Macias; Eliza Liang; Michael Cranfield; Barbara A Han; Morgan W Tingley; Maria Diuk-Wasser; Tracey Goldstein; Christine Kreuder Johnson; Jonna Mazet; Kartik Chandran; Vincent Munster; Kirsten Gilardi; Simon J Anthony.
Afiliación
  • Heather L Wells; Columbia University
  • Michael C Letko; NIH/NIAID
  • Gorka Lasso; Albert Einstein College of Medicine
  • Benard Ssebide; Gorilla Doctors, Wildlife Health Institute, University of California Davis
  • Julius Nziza; Gorilla Doctors, Wildlife Health Institute, University of California Davis
  • Denis K Byarugaba; Makerere University College of Veterinary Medicine
  • Isamara Navarrete-Macias; Columbia University
  • Eliza Liang; Columbia University
  • Michael Cranfield; One Health Institute, Wildlife Health Center, University of California Davis
  • Barbara A Han; Cary Institute of Ecosystem Studies
  • Morgan W Tingley; University of California Los Angeles
  • Maria Diuk-Wasser; Columbia University
  • Tracey Goldstein; One Health Institute, Wildlife Health Center, University of California Davis
  • Christine Kreuder Johnson; One Health Institute, Wildlife Health Center, University of California Davis
  • Jonna Mazet; One Health Institute, Wildlife Health Center, University of California Davis
  • Kartik Chandran; Albert Einstein College of Medicine
  • Vincent Munster; NIAID
  • Kirsten Gilardi; One Health Institute, Wildlife Health Center, University of California Davis
  • Simon J Anthony; University of California Davis
Preprint en Inglés | bioRxiv | ID: ppbiorxiv-190546
ABSTRACT
SARS-CoV-1 and SARS-CoV-2 are not phylogenetically closely related; however, both use the ACE2 receptor in humans for cell entry. This is not a universal sarbecovirus trait; for example, many known sarbecoviruses related to SARS-CoV-1 have two deletions in the receptor binding domain of the spike protein that render them incapable of using human ACE2. Here, we report three sequences of a novel sarbecovirus from Rwanda and Uganda which are phylogenetically intermediate to SARS-CoV-1 and SARS-CoV-2 and demonstrate via in vitro studies that they are also unable to utilize human ACE2. Furthermore, we show that the observed pattern of ACE2 usage among sarbecoviruses is best explained by recombination not of SARS-CoV-2, but of SARS-CoV-1 and its relatives. We show that the lineage that includes SARS-CoV-2 is most likely the ancestral ACE2-using lineage, and that recombination with at least one virus from this group conferred ACE2 usage to the lineage including SARS-CoV-1 at some time in the past. We argue that alternative scenarios such as convergent evolution are much less parsimonious; we show that biogeography and patterns of host tropism support the plausibility of a recombination scenario; and we propose a competitive release hypothesis to explain how this recombination event could have occurred and why it is evolutionarily advantageous. The findings provide important insights into the natural history of ACE2 usage for both SARS-CoV-1 and SARS-CoV-2, and a greater understanding of the evolutionary mechanisms that shape zoonotic potential of coronaviruses. This study also underscores the need for increased surveillance for sarbecoviruses in southwestern China, where most ACE2-using viruses have been found to date, as well as other regions such as Africa, where these viruses have only recently been discovered.
Licencia
cc_by_nc_nd
Texto completo: Disponible Colección: Preprints Base de datos: bioRxiv Tipo de estudio: Estudio pronóstico Idioma: Inglés Año: 2020 Tipo del documento: Preprint
Texto completo: Disponible Colección: Preprints Base de datos: bioRxiv Tipo de estudio: Estudio pronóstico Idioma: Inglés Año: 2020 Tipo del documento: Preprint
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