Human Vaccines & Immunotherapeutics (Feb 2020)

In silico identification and modification of T cell epitopes in pertussis antigens associated with tolerance

  • Corine Kruiswijk,
  • Guilhem Richard,
  • Merijn L.M. Salverda,
  • Pooja Hindocha,
  • William D. Martin,
  • Anne S. De Groot,
  • Elly Van Riet

DOI
https://doi.org/10.1080/21645515.2019.1703453
Journal volume & issue
Vol. 16, no. 2
pp. 277 – 285

Abstract

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The resurgence of whooping cough since the introduction of acellular (protein) vaccines has led to a renewed interest in the development of improved pertussis vaccines; Outer Membrane Vesicles (OMVs) carrying pertussis antigens have emerged as viable candidates. An in silico immunogenicity screen was carried out on 49 well-known Bordetella pertussis proteins in order to better understand their potential role toward the efficacy of pertussis OMVs for vaccine design; seven proteins were identified as being good candidates for including in optimized cellular and acellular pertussis vaccines. We then screened these antigens for putative tolerance-inducing sequences, as proteins with reduced tolerogenicity have improved vaccine potency in preclinical models. We used specialized homology tools (JanusMatrix) to identify peptides in the proteins that were cross-reactive with human sequences. Four of the 19 identified cross-reactive peptides were detolerized in silico using a separate tool, OptiMatrix, which disrupted the potential of these peptides to bind to human HLA and murine MHC. Four selected cross-reactive peptides and their detolerized variants were synthesized and their binding to a set of eight common HLA class II alleles was assessed in vitro. Reduced binding affinity to HLA class II was observed for the detolerized variants compared to the wild-type peptides, highlighting the potential of this approach for designing more efficacious pertussis vaccines.

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