4.8 Article

The Route of Vaccine Administration Determines Whether Blood Neutrophils Undergo Long-Term Phenotypic Modifications

Journal

FRONTIERS IN IMMUNOLOGY
Volume 12, Issue -, Pages -

Publisher

FRONTIERS MEDIA SA
DOI: 10.3389/fimmu.2021.784813

Keywords

vaccine; innate immunity; innate immune memory; trained immunity; Modified vaccinia virus Ankara (MVA); administration routes; mass cytometry (CyTOF)

Categories

Funding

  1. IDMIT infrastructure
  2. ANR [ANR-11-INBS-0008]
  3. Investissements d'Avenir programs [ANR10-LABX-77-01, ANR-10-EQPX-02-01]
  4. European Commission [FP7-HEALTH-2011-280873]
  5. Transvac, EU H2020 [GA 730964]
  6. EHVA, EU H2020 [GA 681032]
  7. ANRS (France Recherche Nord&Sud Sida-HIV Hepatites)

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The study demonstrates that different routes of immunization can lead to distinct innate cell responses, influencing the immune effects of vaccines. The vaccine per se is not enough to induce late phenotypic modifications of innate myeloid cells, emphasizing the importance of the route of administration in vaccination.
Innate immunity modulates adaptive immunity and defines the magnitude, quality, and longevity of antigen-specific T- and B- cell immune memory. Various vaccine and administration factors influence the immune response to vaccination, including the route of vaccine delivery. We studied the dynamics of innate cell responses in blood using a preclinical model of non-human primates immunized with a live attenuated vaccinia virus, a recombinant Modified vaccinia virus Ankara (MVA) expressing a gag-pol-nef fusion of HIV-1, and mass cytometry. We previously showed that it induces a strong, early, and transient innate response, but also late phenotypic modifications of blood myeloid cells after two months when injected subcutaneously. Here, we show that the early innate effector cell responses and plasma inflammatory cytokine profiles differ between subcutaneous and intradermal vaccine injection. Additionally, we show that the intradermal administration fails to induce more highly activated/mature neutrophils long after immunization, in contrast to subcutaneous administration. Different batches of antibodies, staining protocols and generations of mass cytometers were used to generate the two datasets. Mass cytometry data were analyzed in parallel using the same analytical pipeline based on three successive clustering steps, including SPADE, and categorical heatmaps were compared using the Manhattan distance to measure the similarity between cell cluster phenotypes. Overall, we show that the vaccine per se is not sufficient for the late phenotypic modifications of innate myeloid cells, which are evocative of innate immune training. Its route of administration is also crucial, likely by influencing the early innate response, and systemic inflammation, and vaccine biodistribution.

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