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Mapping the interaction sites of human and avian influenza A viruses and complement factor H.
Rabeeah, Iman; Billington, Elizabeth; Nal, Béatrice; Sadeyen, Jean-Remy; Pathan, Ansar A; Iqbal, Munir; Temperton, Nigel J; Zipfel, Peter F; Skerka, Christine; Kishore, Uday; Shelton, Holly.
Affiliation
  • Rabeeah I; Pirbright Institute, Woking, United Kingdom.
  • Billington E; Biosciences, College of Health, Medicine and Life Sciences, Brunel University London, Uxbridge, United Kingdom.
  • Nal B; Pirbright Institute, Woking, United Kingdom.
  • Sadeyen JR; Aix-Marseille Université, CNRS, INSERM, CIML, Marseille, France.
  • Pathan AA; Pirbright Institute, Woking, United Kingdom.
  • Iqbal M; Biosciences, College of Health, Medicine and Life Sciences, Brunel University London, Uxbridge, United Kingdom.
  • Temperton NJ; Pirbright Institute, Woking, United Kingdom.
  • Zipfel PF; Viral Pseudotype Unit, University of Kent, Chatham, United Kingdom.
  • Skerka C; Department of Infection Biology, Leibniz Institute for Natural Product Research and Infection Biology, Jena, Germany.
  • Kishore U; Institute of Microbiology, Friedrich Schiller University, Jena, Germany.
  • Shelton H; Department of Infection Biology, Leibniz Institute for Natural Product Research and Infection Biology, Jena, Germany.
Front Immunol ; 15: 1352022, 2024.
Article in En | MEDLINE | ID: mdl-38698856
ABSTRACT
The complement system is an innate immune mechanism against microbial infections. It involves a cascade of effector molecules that is activated via classical, lectin and alternative pathways. Consequently, many pathogens bind to or incorporate in their structures host negative regulators of the complement pathways as an evasion mechanism. Factor H (FH) is a negative regulator of the complement alternative pathway that protects "self" cells of the host from non-specific complement attack. FH has been shown to bind viruses including human influenza A viruses (IAVs). In addition to its involvement in the regulation of complement activation, FH has also been shown to perform a range of functions on its own including its direct interaction with pathogens. Here, we show that human FH can bind directly to IAVs of both human and avian origin, and the interaction is mediated via the IAV surface glycoprotein haemagglutinin (HA). HA bound to common pathogen binding footprints on the FH structure, complement control protein modules, CCP 5-7 and CCP 15-20. The FH binding to H1 and H3 showed that the interaction overlapped with the receptor binding site of both HAs, but the footprint was more extensive for the H3 HA than the H1 HA. The HA - FH interaction impeded the initial entry of H1N1 and H3N2 IAV strains but its impact on viral multicycle replication in human lung cells was strain-specific. The H3N2 virus binding to cells was significantly inhibited by preincubation with FH, whereas there was no alteration in replicative rate and progeny virus release for human H1N1, or avian H9N2 and H5N3 IAV strains. We have mapped the interaction between FH and IAV, the in vivo significance of which for the virus or host is yet to be elucidated.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Influenza A virus / Protein Binding / Complement Factor H / Hemagglutinin Glycoproteins, Influenza Virus / Influenza, Human Limits: Animals / Humans Language: En Journal: Front Immunol Year: 2024 Document type: Article Affiliation country: Reino Unido Country of publication: Suiza

Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Influenza A virus / Protein Binding / Complement Factor H / Hemagglutinin Glycoproteins, Influenza Virus / Influenza, Human Limits: Animals / Humans Language: En Journal: Front Immunol Year: 2024 Document type: Article Affiliation country: Reino Unido Country of publication: Suiza