Scientific Reports (Aug 2017)

Enhancing Immune Responses to Cancer Vaccines Using Multi-Site Injections

  • Robert C. Mould,
  • Amanda W. K. AuYeung,
  • Jacob P. van Vloten,
  • Leonardo Susta,
  • Anthony J. Mutsaers,
  • James J. Petrik,
  • Geoffrey A. Wood,
  • Sarah K. Wootton,
  • Khalil Karimi,
  • Byram W. Bridle

DOI
https://doi.org/10.1038/s41598-017-08665-9
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 8

Abstract

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Abstract For a vaccine to be effective it must induce a sufficiently robust and specific immune response. Multi-site injection protocols can increase the titers of rabies virus-neutralizing antibodies. Hypothetically, spreading a vaccine dose across multiple lymphatic drainage regions could also potentiate T cell responses. We used a replication-deficient adenovirus serotype 5-vectored cancer vaccine targeting the melanoma-associated antigen dopachrome tautomerase. Clinically, high numbers of tumor-infiltrating CD8+ T cells are a positive prognostic indicator. As such, there is interest in maximizing tumor-specific T cell responses. Our findings confirm a positive correlation between the number of tumor-specific T cells and survival. More importantly, we show for the first time that using multiple injection sites could increase the number of vaccine-induced CD8+ T cells specific for a self-tumor antigen. Further, the number of tumor antigen-specific antibodies, as well CD8+ T cells specific for a foreign antigen could also be enhanced. Our results show that multi-site vaccination induces higher magnitude immune responses than a single-bolus injection. This provides a very simple and almost cost-free strategy to potentially improve the efficacy of any current and future vaccine. Broader clinical adoption of multi-site vaccination protocols for the treatment of cancers and infectious diseases should be given serious consideration.