Glyco-engineered MDCK cells display preferred receptors of H3N2 influenza absent in eggs used for vaccines

糖基工程 MDCK 细胞表现出 H3N2 流感病毒的优先受体,而疫苗所用的鸡蛋中却没有这种受体

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作者:Chika Kikuchi #, Aristotelis Antonopoulos #, Shengyang Wang, Tadashi Maemura, Rositsa Karamanska, Chiara Lee, Andrew J Thompson, Anne Dell, Yoshihiro Kawaoka, Stuart M Haslam, James C Paulson

Abstract

Evolution of human H3N2 influenza viruses driven by immune selection has narrowed the receptor specificity of the hemagglutinin (HA) to a restricted subset of human-type (Neu5Acα2-6 Gal) glycan receptors that have extended poly-LacNAc (Galβ1-4GlcNAc) repeats. This altered specificity has presented challenges for hemagglutination assays, growth in laboratory hosts, and vaccine production in eggs. To assess the impact of extended glycan receptors on virus binding, infection, and growth, we have engineered N-glycan extended (NExt) cell lines by overexpressing β3-Ν-acetylglucosaminyltransferase 2 in MDCK, SIAT, and hCK cell lines. Of these, SIAT-NExt cells exhibit markedly increased binding of H3 HAs and susceptibility to infection by recent H3N2 virus strains, but without impacting final virus titers. Glycome analysis of these cell lines and allantoic and amniotic egg membranes provide insights into the importance of extended glycan receptors for growth of recent H3N2 viruses and relevance to their production for cell- and egg-based vaccines.

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