Sialic acid removal from dendritic cells improves antigen cross-presentation and boosts anti-tumor immune responses

  • Mariana Silva
  • , Zélia Silva
  • , Graça Marques
  • , Tiago Ferro
  • , Márcia Gonçalves
  • , Mauro Monteiro
  • , Sandra J. van Vliet
  • , Elodie Mohr
  • , Andreia C. Lino
  • , Alexandra R. Fernandes
  • , Flávia A. Lima
  • , Yvette van Kooyk
  • , Teresa Matos
  • , Carlos E. Tadokoro
  • , Paula A. Videira

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45 Citações (Scopus)

Resumo

Dendritic cells (DCs) hold promise for anti-cancer immunotherapy. However, clinically, their efficiency is limited and novel strategies to improve DC-mediated anti-tumor responses are needed. Human DCs display high content of sialic acids, which inhibits their maturation and co-stimulation capacity. Here, we aimed to understand whether exogenous desialylation of DCs improves their anti-tumor immunity. Compared to fully sialylated DCs, desialylated human DCs loaded with tumor-antigens showed enhanced ability to induce autologous T cells to proliferate, to secrete Th1 cytokines, and to specifically induce tumor cell apoptosis. Desialylated DCs showed an increased expression of MHC-I and -II, co-stimulatory molecules and an augmented secretion of IL-12. Desialylated HLA-A*02:01 DCs pulsed with gp100 peptides displayed enhanced peptide presentation through MHC-I, resulting in higher activation ofgp100280-288 specific CD8+ cytotoxic T cells. Desialylated murine DCs also exhibited increased MHC and co-stimulatory molecules and higher antigen cross-presentation via MHC-I. These DCs showed higher ability to activate antigen-specific CD4+ and CD8+ T cells, and to specifically induce tumor cell apoptosis. Collectively, our data demonstrates that desialylation improves DCs' ability to elicit T cell-mediated anti-tumor activity, due to increased MHC-I expression and higher antigen presentation via MHC-I. Sialidase treatment of DCs may represent a technology to improve the efficacy of antigen loaded-DC-based vaccines for anti-cancer immunotherapy.

Idioma original???core.languages.en_GB???
Páginas (de-até)41053-41066
Número de páginas14
RevistaOncotarget
Volume7
Número de emissão27
DOIs
Estado da publicação???researchoutput.status.published??? - 5 jul. 2016
Publicado externamenteSim

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