In Vivo Targeting of Antigens to Maturing Dendritic Cells via the DEC-205 Receptor Improves T Cell Vaccination

Laura C. Bonifaz(Rockefeller University), David Bonnyay(Rockefeller University), Anna Charalambous(Rockefeller University), Dara I. Darguste(Rockefeller University), Shin‐ichiro Fujii(Rockefeller University), Helena Soares(Rockefeller University), Marie K. Brimnes(Icahn School of Medicine at Mount Sinai), Bruno Moltedo(Icahn School of Medicine at Mount Sinai), Thomas M. Moran(Icahn School of Medicine at Mount Sinai), Ralph M. Steinman(Rockefeller University)
The Journal of Experimental Medicine
March 15, 2004
Cited by 906Open Access
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Abstract

The prevention and treatment of prevalent infectious diseases and tumors should benefit from improvements in the induction of antigen-specific T cell immunity. To assess the potential of antigen targeting to dendritic cells to improve immunity, we incorporated ovalbumin protein into a monoclonal antibody to the DEC-205 receptor, an endocytic receptor that is abundant on these cells in lymphoid tissues. Simultaneously, we injected agonistic alpha-CD40 antibody to mature the dendritic cells. We found that a single low dose of antibody-conjugated ovalbumin initiated immunity from the naive CD4+ and CD8+ T cell repertoire. Unexpectedly, the alphaDEC-205 antigen conjugates, given s.c., targeted to dendritic cells systemically and for long periods, and ovalbumin peptide was presented on MHC class I for 2 weeks. This was associated with stronger CD8+ T cell-mediated immunity relative to other forms of antigen delivery, even when the latter was given at a thousand times higher doses. In parallel, the mice showed enhanced resistance to an established rapidly growing tumor and to viral infection at a mucosal site. By better harnessing the immunizing functions of maturing dendritic cells, antibody-mediated antigen targeting via the DEC-205 receptor increases the efficiency of vaccination for T cell immunity, including systemic and mucosal resistance in disease models.


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