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Heat-Shock Induction of Tumor-Derived Danger Signals Mediates Rapid Monocyte Differentiation into Clinically Effective Dendritic Cells

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2011-04-15
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Aguilera, Raquel
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Heat-Shock Induction of Tumor-Derived Danger Signals Mediates Rapid Monocyte Differentiation into Clinically Effective Dendritic Cells
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Author
  • Aguilera, Raquel;
  • Saffie, Carlos;
  • Tittarelli, Andrés;
  • González Bergas, Fermín;
  • Ramírez Fernández, Marcos;
  • Reyes, Diego;
  • Pereda, Cristián;
  • Hevia, Daniel;
  • García, Tamara;
  • Salazar, Lorena;
  • Ferreira Vigouroux, Luis Arturo;
  • Hermoso Ramello, Marcela;
  • Mendoza Naranjo, Ariadna;
  • Ferrada, Carlos;
  • Garrido, Paola;
  • López Nitsche, Mercedes;
  • Salazar Onfray, Flavio;
Abstract
Purpose: This study characterizes, biologically and clinically, a novel type of dendritic cells (DC) produced in the short term and called tumor antigen–presenting cells (TAPCells). In particular, we identified factors present in a lysate derived from heat-shocked allogeneic melanoma cells (TRIMEL) that are associated with TAPCells’ enhanced capability to induce CD8þ T-cell responses in vitro and in vaccinated melanoma patients. Experimental Design: First, extensive phenotypic and functional characterization of TAPCells was performed, followed by vaccination of 45 melanoma patients with four doses of TAPCells over a period of 2 months. Specific delayed-type hypersensitivity (DTH) reaction was analyzed posttreatment and correlated with overall survival rates. Furthermore, heat-shock (HS)-induced factors present in TRIMEL and their effects on DC activation were identified and studied. Results: TRIMEL induced a committed, mature, DC-like phenotype in TAPCells and effectively activated melanoma-specific CD4þ and CD8þ T cells. Clinically, 64% of vaccinated patients showed positive DTH reaction against TRIMEL, and this was associated with improved overall survival. HS treatment of tumor cells increased calreticulin (CRT) plasma membrane translocation and induced the release of high-mobility group box 1 proteins (HMGB1). Both CRT and HMGB1 mobilization were associated with enhanced TAPCells’ maturation and antigen (Ag) cross-presentation, respectively. DTH infiltration analysis revealed the presence of CD8þ/CD45ROþ T cells, thus confirming TAPCells’ ability to cross-present Ags in vivo. Conclusions: Our results indicate that lysates derived fromheat-shocked tumor cells are an optimal source of tumor-associated Ags, which are crucial for the generation of DCs with improved Ag cross-presentation capacity and clinically effective immunogenicity.
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This work was supported by grants from the National Fund for Scientific and Technological Development (FONDECYT 1090238, 1090243, 3090044), the Fund for the Promotion of Scientific and Technological Development (FONDEF DO5I10366), and the Millennium Nucleus of Immunology and Immunotherapy (P04/030-F).
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URI: https://repositorio.uchile.cl/handle/2250/128861
DOI: DOI: 10.1158/1078-0432.CCR-10-2384
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CLINICAL CANCER RESEARCH Volume: 17 Issue: 8 Pages: 2474-2483 Published: APR 15 2011
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