Antibodies targeting the neuraminidase active site inhibit influenza H3N2 viruses with an S245N glycosylation site.
Daniel StadlbauerMeagan McMahonHannah L TurnerXueyong ZhuHongquan WanJuan Manuel CarreñoGeorge O'DellShirin StrohmeierZain KhalilMarta LukszaHarm van BakelViviana SimonAli H EllebedyIan A WilsonAndrew B WardFlorian KrammerPublished in: Nature communications (2022)
Contemporary influenza A H3N2 viruses circulating since 2016 have acquired a glycosylation site in the neuraminidase in close proximity to the enzymatic active site. Here, we investigate if this S245N glycosylation site, as a result of antigenic evolution, can impact binding and function of human monoclonal antibodies that target the conserved active site. While we find that a reduction in the inhibitory ability of neuraminidase active site binders is measurable, this class of broadly reactive monoclonal antibodies maintains protective efficacy in vivo.