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[Preprint]. 2024 Feb 26:2023.10.26.23297569. Originally published 2023 Oct 27. [Version 2] doi: 10.1101/2023.10.26.23297569

PMC10635207.1; 2023 Oct 27
PMC10635207.2; 2024 Feb 26
PMC10635207.3; 2024 May 21
PMC10635207.4; 2024 Jul 8
PMC10635207.5; 2024 Oct 10

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Fig 1. — A. Genealogies of H3N2 HA through the 2016–2017 (left) and 2017–2018 season (right). Branches are colored by clade. Tips are shown as filled circles if collected in North America during the most recent season. B. Amino acid and glycosylation site variation among reference viruses. Clades 3C.3A and 3C.2A diverge at additional non-epitope sites (not shown). Residue 128 belongs to antigenic site B, but the substitution T128A results in loss of glycosylation on residue 126 of epitope A. Therefore, we show residue 128 in epitope A and in the glycosylation site involving residues 126–128, following [1]. C. Variable residues among the reference viruses are shown on the H3 structure of A/Aichi/2/1968 (Protein Data Bank: 1HGG) and colored by epitope as in panel B. For each strain, residues differing from 3C.2A are numbered and darker in color. D. Glycosylation sites used in the model shown on the H3 structure.