Tumors hamper the immunogenic competence of CD4+ T cell-directed dendritic cell vaccination

VS Zimmermann, A Casati, C Schiering… - The Journal of …, 2007 - journals.aai.org
VS Zimmermann, A Casati, C Schiering, S Caserta, R Hess Michelini, V Basso, A Mondino
The Journal of Immunology, 2007journals.aai.org
Dendritic cells loaded with tumor-derived peptides induce protective CTL responses and are
under evaluation in clinical trails. We report in this study that prophylactic administration of
dendritic cells loaded with a MHC class II-restricted peptide derived from a model tumor Ag
(Leishmania receptor for activated C kinase (LACK)) confers protection against LACK-
expressing TS/A tumors, whereas therapeutic vaccination fails to cure tumor-bearing mice.
Although CD4+ T cell-directed dendritic cell vaccination primed effector-like (CD44 high …
Abstract
Dendritic cells loaded with tumor-derived peptides induce protective CTL responses and are under evaluation in clinical trails. We report in this study that prophylactic administration of dendritic cells loaded with a MHC class II-restricted peptide derived from a model tumor Ag (Leishmania receptor for activated C kinase (LACK)) confers protection against LACK-expressing TS/A tumors, whereas therapeutic vaccination fails to cure tumor-bearing mice. Although CD4+ T cell-directed dendritic cell vaccination primed effector-like (CD44 high CD62L low, IL-2+, IFN-γ+) and central memory-like lymphocytes (CD44 high CD62L high, only IL-2+) in tumor-free mice, this was not the case in tumor-bearing animals in which both priming and persistence of CD4+ T cell memory were suppressed. Suppression was specific for the tumor-associated Ag LACK, and did not depend on CD25+ T cells. Because T cell help is needed for protective immunity, we speculate that the ability of tumors to limit vaccine-induced CD4+ T cell memory could provide a partial explanation for the limited efficacy of current strategies.
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