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Lymphocytes genetically modified to express tumor antigens target DCs in vivo and induce antitumor immunity

Articolo
Data di Pubblicazione:
2007
Abstract:
The exploitation of the physiologic processing and presenting machinery of DCs by in vivo loading of tumor-associated antigens may improve the immunogenic potential and clinical efficacy of DC-based cancer vaccines. Here we show that lymphocytes genetically modified to express self/tumor antigens, acting as antigen carriers, efficiently target DCs in vivo in tumor-bearing mice. The infusion of tyrosinase-related protein 2-transduced (TRP-2-transduced) lymphocytes induced the establishment of protective immunity and long-term memory in tumor-bearing mice. Analysis of the mechanism responsible for the induction of such an immune response allowed us to demonstrate that cross-presentation of the antigen mediated by the CD11c(+)CD8 alpha(+) DC subset had occurred. Furthermore, we demonstrated in vivo and in vitro that DCs had undergone activation upon phagocytosis of genetically modified lymphocytes, a process mediated by a cell-to-cell contact mechanism independent of CD40 triggering. Targeting and activation of secondary lymphoid organ-resident DCs endowed antigen-specific T cells with full effector functions, which ultimately increased tumor growth control and animal survival in a therapeutic tumor setting. We conclude that the use of transduced lymphocytes represents an efficient method for the in vivo loading of tumor-associated antigens on DCs.
Tipologia CRIS:
1.1 Articolo in rivista
Elenco autori:
Russo, V; Cipponi, A; Raccosta, L; Rainelli, C; Fontana, R; Maggioni, D; Lunghi, F; Mukenge, S; Ciceri, Fabio; Bregni, M; Bordignon, Claudio; Traversari, C.
Autori di Ateneo:
CICERI FABIO
RUSSO VINCENZO
Link alla scheda completa:
https://iris.unisr.it/handle/20.500.11768/10987
Pubblicato in:
THE JOURNAL OF CLINICAL INVESTIGATION
Journal
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