Glycan remodeled erythrocytes facilitate antigenic characterization of recent A/H3N2 influenza viruses

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作者
Frederik Broszeit
Rosanne J. van Beek
Luca Unione
Theo M. Bestebroer
Digantkumar Chapla
Jeong-Yeh Yang
Kelley W. Moremen
Sander Herfst
Ron A. M. Fouchier
Robert P. de Vries
Geert-Jan Boons
机构
[1] Utrecht University,Department of Chemical Biology & Drug Discovery, Utrecht Institute for Pharmaceutical Sciences
[2] Erasmus MC,Department of Viroscience
[3] University of Georgia,Complex Carbohydrate Research Center
[4] Utrecht University,Bijvoet Center for Biomolecular Research
[5] University of Georgia,Department of Chemistry
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During circulation in humans and natural selection to escape antibody recognition for decades, A/H3N2 influenza viruses emerged with altered receptor specificities. These viruses lost the ability to agglutinate erythrocytes critical for antigenic characterization and give low yields and acquire adaptive mutations when cultured in eggs and cells, contributing to recent vaccine challenges. Examination of receptor specificities of A/H3N2 viruses reveals that recent viruses compensated for decreased binding of the prototypic human receptor by recognizing α2,6-sialosides on extended LacNAc moieties. Erythrocyte glycomics shows an absence of extended glycans providing a rationale for lack of agglutination by recent A/H3N2 viruses. A glycan remodeling approach installing functional receptors on erythrocytes, allows antigenic characterization of recent A/H3N2 viruses confirming the cocirculation of antigenically different viruses in humans. Computational analysis of HAs in complex with sialosides having extended LacNAc moieties reveals that mutations distal to the RBD reoriented the Y159 side chain resulting in an extended receptor binding site.
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