par Moulin, Véronique 
;Andris, Fabienne ;Thielemans, Kris M.;Maliszewski, Charles;Urbain, Jacques ;Moser, Muriel
Référence The Journal of experimental medicine, 192, 4, page (475-482)
Publication Publié, 2000-08
;Andris, Fabienne ;Thielemans, Kris M.;Maliszewski, Charles;Urbain, Jacques ;Moser, Muriel Référence The Journal of experimental medicine, 192, 4, page (475-482)
Publication Publié, 2000-08
Article révisé par les pairs
| Résumé : | Increasing evidence indicates that dendritic cells (DCs) are the antigen-presenting cells of the primary immune response. However, several reports suggest that B lymphocytes could be required for optimal T cell sensitization. We compared the immune responses of wild-type and B cell-deficient (muMT) mice, induced by antigen emulsified in adjuvant or pulsed on splenic dendritic cells. Our data show that lymph node cells from both control and muMT animals were primed, but each released distinct cytokine profiles. Lymph node T cells from control animals secreted interferon (IFN)-gamma, interleukin (IL)-2, and IL-4, whereas those from muMT mice produced IFN-gamma and IL-2 but no IL-4. To test whether B cells may influence the T helper cell type 1 (Th1)/Th2 balance by affecting the function of DCs, we immunized mice by transferring antigen-pulsed DCs from wild-type or mutant mice. Injection of control DCs induced the secretion of IL-4, IFN-gamma, and IL-2, whereas administration of DCs from muMT animals failed to sensitize cells to produce IL-4. Analysis of IL-12 production revealed that DCs from muMT mice produce higher levels of IL-12p70 than do DCs from wild-type animals. These data suggest that B lymphocytes regulate the capacity of DCs to promote IL-4 secretion, possibly by downregulating their secretion of IL-12, thereby favoring the induction of a nonpolarized immune response. |
