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Viral capsid, antibody, and receptor interactions: experimental analysis of the antibody escape evolution of canine parvovirus.

Robert A López-AstacioOluwafemi F AduDaniel J GoetschiusHyunwook LeeWendy S WeichertBrian R WasikSimon P FruehBrynn K AlfordIan E H VoorheesJoseph F FlintSarah SaddorisLaura B GoodmanEdward C HolmesSusan L HafensteinColin R Parrish
Published in: bioRxiv : the preprint server for biology (2023)
model system and deep genome sequencing to reveal the mutations that arise in the virus genome during selection by each of two monoclonal antibodies or their engineered variants. High-resolution structures of each of the Fab: capsid complexes revealed their binding interactions. The engineered forms of the wild-type antibodies or mutant forms allowed us to examine how changes in antibody structure influence the mutational selection patterns seen in the virus. The results shed light on the processes of antibody binding, neutralization escape, and receptor binding, and likely have parallels for many other viruses.
Keyphrases
  • wild type
  • high resolution
  • single cell
  • binding protein
  • genome wide
  • sars cov
  • mass spectrometry
  • copy number