Recent H3N2 Viruses Have Evolved Specificity for Extended, Branched Human-type Receptors, Conferring Potential for Increased Avidity
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文摘
All H3N2 influenza viruses recognize human-type receptors with extended glycan chains Recent H3 and pandemic H1 hemagglutinins prefer extended, branched N-glycan receptors Lipid-linked glycan receptors restore infectivity to receptor-deficient MDCK cells Molecular dynamics simulation shows bidentate binding of N-glycans to one HA trimer

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