| Literature DB >> 35831293 |
Mengying Liu1, Liane Z X Huang1, Anthony A Smits1, Christian Büll2,3, Yoshiki Narimatsu2, Frank J M van Kuppeveld1, Henrik Clausen2, Cornelis A M de Haan4, Erik de Vries5.
Abstract
Establishment of zoonotic viruses, causing pandemics like the Spanish flu and Covid-19, requires adaptation to human receptors. Pandemic influenza A viruses (IAV) that crossed the avian-human species barrier switched from binding avian-type α2-3-linked sialic acid (2-3Sia) to human-type 2-6Sia receptors. Here, we show that this specificity switch is however less dichotomous as generally assumed. Binding and entry specificity were compared using mixed synthetic glycan gradients of 2-3Sia and 2-6Sia and by employing a genetically remodeled Sia repertoire on the surface of a Sia-free cell line and on a sialoglycoprotein secreted from these cells. Expression of a range of (mixed) 2-3Sia and 2-6Sia densities shows that non-binding human-type receptors efficiently enhanced avian IAV binding and entry provided the presence of a low density of high affinity avian-type receptors, and vice versa. Considering the heterogeneity of sialoglycan receptors encountered in vivo, hetero-multivalent binding is physiologically relevant and will impact evolutionary pathways leading to host adaptation.Entities:
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Year: 2022 PMID: 35831293 PMCID: PMC9279479 DOI: 10.1038/s41467-022-31840-0
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 17.694