Purification of splenic dendritic cells induces maturation and capacity to stimulate Th1 response in vivo

doi:10.1093/intimm/dxh384

International Immunology Advance Access published online on January 13, 2006
International Immunology, doi:10.1093/intimm/dxh384

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© The Japanese Society for Immunology. 2006. All rights reserved. For permissions, please e-mail: journals.permissions@oxfordjournals.org
Received June 28, 2005
Accepted December 13, 2005

Article

Purification of splenic dendritic cells induces maturation and capacity to stimulate T_h1 response in vivo

Géraldine Schlecht ¹, Juliette Mouriès ¹, Maud Poitrasson-Rivière ¹, Claude Leclerc ¹, and Gilles Dadaglio ¹ ^*

¹ Institut Pasteur, Unité de Biologie des Régulations Immunitaires, Paris F-75015, France; Inserm, E 352, Paris F-75015, France

^* To whom correspondence should be addressed.
Gilles Dadaglio, E-mail: gdadag{at}pasteur.fr

Abstract

Dendritic cell (DC) maturation state is a key parameter forthe issue of DC-T cell cognate interaction, which determinesthe outcome of T cell activation. Indeed, immature DCs inducetolerance while fully mature DCs generate immunity. Here weshow that, in the absence of any deliberate activation signal,DCs freshly isolated from mouse spleen spontaneously produceIL-12 and tumor necrosis factor- ${alpha}$ and up-regulate co-stimulationmolecules, even when directly re-injected into their naturalenvironment. Furthermore, after their isolation, these cellsacquire the capacity to induce specific T_h1 responses in vivo.These results demonstrate that the sole isolation of spleenDCs leads to the full maturation of these cells, which thereforecannot be considered as immature DCs. Moreover, we also showthat the kinetics of DC activation do not influence the polarizationof T_h response in vivo challenging the idea that exhausted DCsinduce preferentially T_h2 response. Altogether, these observationsshould be taken into account in all experiments based on thetransfer of ex vivo purified DCs.

Keywords: activation; antigen-presenting cell; T cell response.

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