Transcutaneous anti-influenza vaccination promotes both CD4 and CD8 T cell immune responses in humans

A Vogt, B Mahé, D Costagliola, O Bonduelle… - The Journal of …, 2008 - journals.aai.org
A Vogt, B Mahé, D Costagliola, O Bonduelle, S Hadam, G Schaefer, H Schaefer, C Katlama…
The Journal of Immunology, 2008journals.aai.org
Induction of T cell responses has become one of the major goals in therapeutic vaccination
against viral diseases and cancer. The use of the skin as target organ for vaccine has been
spurred by recent implication of epithelial dendritic cells in CD8 cell cross-priming and
suggests that vaccination via the transcutaneous (TC) route may be relevant in the induction
of cellular immune responses. We have previously shown that TC application of
nanoparticles, on human skin explants, allows targeting of epidermal dendritic cells …
Abstract
Induction of T cell responses has become one of the major goals in therapeutic vaccination against viral diseases and cancer. The use of the skin as target organ for vaccine has been spurred by recent implication of epithelial dendritic cells in CD8 cell cross-priming and suggests that vaccination via the transcutaneous (TC) route may be relevant in the induction of cellular immune responses. We have previously shown that TC application of nanoparticles, on human skin explants, allows targeting of epidermal dendritic cells, possibly via hair follicles. In this study, we have investigated cellular immune responses against an influenza protein-based vaccine by TC vaccination, compared with im vaccination in humans. In this study on 11 healthy volunteers, we found that a newly developed protocol based on cyanocrylate skin surface stripping induced a significant increase in IFNγ-producing T cells specific for influenza vaccine by ELISPOT assays. Interestingly, TC vaccination induced both effector CD4 and CD8 T cell responses, whereas im injection induced strong effector CD4 in the absence of CD8 T cells, as assessed by intracellular cytokine staining and tetramer analyses. This study proposes new perspectives for the development of vaccination strategies that trigger T cell immune responses in humans.
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