Journal of Experimental & Clinical Cancer Research (Feb 2019)

Poly-specific neoantigen-targeted cancer vaccines delay patient derived tumor growth

  • Luigi Aurisicchio,
  • Erika Salvatori,
  • Lucia Lione,
  • Silvio Bandini,
  • Matteo Pallocca,
  • Roberta Maggio,
  • Maurizio Fanciulli,
  • Francesca De Nicola,
  • Frauke Goeman,
  • Gennaro Ciliberto,
  • Antonella Conforti,
  • Laura Luberto,
  • Fabio Palombo

DOI
https://doi.org/10.1186/s13046-019-1084-4
Journal volume & issue
Vol. 38, no. 1
pp. 1 – 13

Abstract

Read online

Abstract Background Personalized cancer vaccines based on neoantigens have reached the clinical trial stage in melanoma. Different vaccination protocols showed efficacy in preclinical models without a clear indication of the quality and the number of neoantigens required for an effective cancer vaccine. Methods In an effort to develop potent and efficacious neoantigen-based vaccines, we have developed different neoantigen minigene (NAM) vaccine vectors to determine the rules for a successful neoantigen cancer vaccine (NCV) delivered by plasmid DNA and electroporation. Immune responses were analyzed at the level of single neoantigen by flow cytometry and correlated with tumor growth. Adoptive T cell transfer, from HLA-2.1.1 mice, was used to demonstrate the efficacy of the NCV pipeline against human-derived tumors. Results In agreement with previous bodies of evidence, immunogenicity was driven by predicted affinity. A strong poly-functional and poly-specific immune response was observed with high affinity neoantigens. However, only a high poly-specific vaccine vector was able to completely protect mice from subsequent tumor challenge. More importantly, this pipeline - from the selection of neoantigens to vaccine design - applied to a new model of patient derived tumor xenograft resulted in therapeutic treatment. Conclusions These results suggest a feasible strategy for a neoantigen cancer vaccine that is simple and applicable for clinical developments.

Keywords