2023
DOI: 10.1038/s41598-023-33529-w
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Structural characterisation of hemagglutinin from seven Influenza A H1N1 strains reveal diversity in the C05 antibody recognition site

Abstract: Influenza virus (IV) causes several outbreaks of the flu each year resulting in an economic burden to the healthcare system in the billions of dollars. Several influenza pandemics have occurred during the last century and estimated to have caused 100 million deaths. There are four genera of IV, A (IVA), B (IVB), C (IVC), and D (IVD), with IVA being the most virulent to the human population. Hemagglutinin (HA) is an IVA surface protein that allows the virus to attach to host cell receptors and enter the cell. H… Show more

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Cited by 8 publications
(3 citation statements)
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References 58 publications
(71 reference statements)
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“…The sites Sa, Sb and Ca (as defined in (Xu et al 2010)) include more than one VR and therefore exhibit higher variability, although with clear evidence of periodic re-emergence of the same variants. An extensive epitope mapping exercise using escape mutants by Matsuzaki et al (Matsuzaki et al 2014) confirms that the bulk of antibodies are restricted to the Sa, Sb and Ca2 (a part of Ca that includes VR2) but they were also able to identify at least one antibody which included Ca2 and position 147 (corresponding to OREO) and also a “broadly neutralising” monoclonal antibody (n2) centred on the RBS similar to those described above (Tsibane et al 2012; Krause et al 2011; Whittle et al 2011; Ghafoori et al 2023; Ekiert et al 2012). By contrast, the monoclonal antibody 2D1, derived from B cells of survivors of the 1918 H1N1 pandemic (Xu et al 2010), is highly diverse on account of possessing a footprint that spans 5 VRs; consequently it has low affinity for all strains except 2009 H1 HA (CA04) which is identical in every single residue.…”
Section: Discussionmentioning
confidence: 70%
See 1 more Smart Citation
“…The sites Sa, Sb and Ca (as defined in (Xu et al 2010)) include more than one VR and therefore exhibit higher variability, although with clear evidence of periodic re-emergence of the same variants. An extensive epitope mapping exercise using escape mutants by Matsuzaki et al (Matsuzaki et al 2014) confirms that the bulk of antibodies are restricted to the Sa, Sb and Ca2 (a part of Ca that includes VR2) but they were also able to identify at least one antibody which included Ca2 and position 147 (corresponding to OREO) and also a “broadly neutralising” monoclonal antibody (n2) centred on the RBS similar to those described above (Tsibane et al 2012; Krause et al 2011; Whittle et al 2011; Ghafoori et al 2023; Ekiert et al 2012). By contrast, the monoclonal antibody 2D1, derived from B cells of survivors of the 1918 H1N1 pandemic (Xu et al 2010), is highly diverse on account of possessing a footprint that spans 5 VRs; consequently it has low affinity for all strains except 2009 H1 HA (CA04) which is identical in every single residue.…”
Section: Discussionmentioning
confidence: 70%
“…One possibility is that they are the targets of antibodies of smaller footprint than the typical 700–900Å. Small footprint size may be achieved by the selective dominance of a single complementarity-determining region (CDR) loop as has been demonstrated for monoclonal antibodies such as CO5 (Ekiert et al 2012; Ghafoori et al 2023) and CH65 (Whittle et al 2011). Both contain the VR1 portion of OREO as well as the final residue of VR2.…”
Section: Discussionmentioning
confidence: 99%
“…Polar residue N-95 (HA2) is also observed to interact with the top-scoring ligands. It is vital to take note of the fact that these interacting residues are part of the highly conserved heptad repeat region found close to the fusion peptide (Sriwilaijaroen & Suzuki, 2012; Ghafoori et al, 2023). Such heptad repeats are a common feature observed in amino acid sequences of fusion glycoproteins of several viruses, such as paramyxoviruses, and retroviruses (Chambers et al, 1990).…”
Section: Resultsmentioning
confidence: 99%