PLoS Pathogens (Apr 2021)

High-throughput, single-copy sequencing reveals SARS-CoV-2 spike variants coincident with mounting humoral immunity during acute COVID-19.

  • Sung Hee Ko,
  • Elham Bayat Mokhtari,
  • Prakriti Mudvari,
  • Sydney Stein,
  • Christopher D Stringham,
  • Danielle Wagner,
  • Sabrina Ramelli,
  • Marcos J Ramos-Benitez,
  • Jeffrey R Strich,
  • Richard T Davey,
  • Tongqing Zhou,
  • John Misasi,
  • Peter D Kwong,
  • Daniel S Chertow,
  • Nancy J Sullivan,
  • Eli A Boritz

DOI
https://doi.org/10.1371/journal.ppat.1009431
Journal volume & issue
Vol. 17, no. 4
p. e1009431

Abstract

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Tracking evolution of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) within infected individuals will help elucidate coronavirus disease 2019 (COVID-19) pathogenesis and inform use of antiviral interventions. In this study, we developed an approach for sequencing the region encoding the SARS-CoV-2 virion surface proteins from large numbers of individual virus RNA genomes per sample. We applied this approach to the WA-1 reference clinical isolate of SARS-CoV-2 passaged in vitro and to upper respiratory samples from 7 study participants with COVID-19. SARS-CoV-2 genomes from cell culture were diverse, including 18 haplotypes with non-synonymous mutations clustered in the spike NH2-terminal domain (NTD) and furin cleavage site regions. By contrast, cross-sectional analysis of samples from participants with COVID-19 showed fewer virus variants, without structural clustering of mutations. However, longitudinal analysis in one individual revealed 4 virus haplotypes bearing 3 independent mutations in a spike NTD epitope targeted by autologous antibodies. These mutations arose coincident with a 6.2-fold rise in serum binding to spike and a transient increase in virus burden. We conclude that SARS-CoV-2 exhibits a capacity for rapid genetic adaptation that becomes detectable in vivo with the onset of humoral immunity, with the potential to contribute to delayed virologic clearance in the acute setting.