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Mapping Polyclonal Antibody Responses to Infection Using Next-Generation Phage Display.

Maria T TsoumpeliAnitha VargheseJonathan P OwenBen C MaddisonJanet M DalyKevin C Gough
Published in: Methods in molecular biology (Clifton, N.J.) (2023)
Peptide phage display has historically been used to epitope map monoclonal antibodies. More recently, by coupling this method with next-generation sequencing (so-called next-generation phage display, NGPD) to mass screen peptide binding events, the methodology has been successfully applied to map polyclonal antibody responses to infection. This leads to the identification of panels of mimotopes that represent the pathogen's epitopes. One potential advantage of using such an approach is that the mimotopes can represent not just linear epitopes but also conformational epitopes or those produced from post-translational modifications of proteins or from other non-protein macromolecules. The mapping of such complex immunological recognition of a pathogen can inform novel serological assay development and vaccine design. Here, we provide detailed methods for the application of NGPD to identify panels of mimotopes that are recognized specifically by antibodies from individuals with a particular infection.
Keyphrases
  • pseudomonas aeruginosa
  • high density
  • high resolution
  • high throughput
  • molecular dynamics
  • gene expression
  • binding protein
  • single molecule
  • small molecule
  • room temperature
  • transition metal