Home Helminths (including anthelmintic resistance) [Expression system] Expression system for subunit vaccine
Helminths (including anthelmintic resistance) roadmap:
Vaccines

Roadmap for nematode vaccine development

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10

Expression system

Expression system for subunit vaccine

Research Question

Development of an affordable stable expression system for large-scale production of recombinant protein/glycoproteins

Research Gaps and Challenges

  • That expressed antigens have the correct conformation and glycosylation to induce protective immunity.
  • Generation of stable genetically modified organisms allowing large scale production.
  • Different antigens may require different expression systems

Solution Routes

  • Various cell line expression systems – bacteria, insect, yeast, mammalian, parasite or plant-derived.
  • Epitope mapping to identify minimum required peptides for immune stimulation.
  • Concatamerisation of minimum required epitopes for expression

Dependencies

  • Identity of the protective antigens for the different parasite species.
  • Knowledge of the importance of conformation and secondary modifications (e.g. glycosylation) for protective properties of vaccine antigens.
  • Freedom to operate and/or licensing of vectors and expression cell lines for commercial exploitation

State Of the Art

  • The H. contortus ES antigen Hc23 expressed in E. coli protected lambs against experimental challenge (Alunda lab, Madrid)
  • A vaccine cocktail of eight recombinant T. circumcincta antigens expressed in E.coli and P. pastoris protected lambs and ewes against a trickle challenge (Nisbet et al., 2013, 2016.)
  • C. elegans expression system (Britton et al., Glasgow), active proteases (H11) but non-protective vs. Haemonchus
  • Ostertagia and Cooperia ASPs, recombinant antigens did not protect