In this study, T or NK cell clones used as antigen-presenting cells (T- or NK-APC) were shown to he significantly less efficient than professional APC in inducing Th1 and Th2 cytokines by antigen-specific T cell clones. This phenomenon was not related to a limited engagement of TCR by T-APC, since comparable thresholds of TCR down-regulation were shown when antigen was presented by either T-APC or professional APC. Rather, the stimulatory T-APC weakness was due to their inability, because they are CD40(-), to provide the appropriate co-stimuli to responder T cells both indirectly via IL-12, and partially via direct CD40L triggering on T cells. Indeed, the simultaneous addition of IL-12 and reagents directly engaging CD40L on responder T cells restored T cell cytokine synthesis when antigen was presented by T-APC. In addition, either IL-12 production or blocking of T cell cytokine synthesis by anti-IL-12 p75 antibodies was evident only when professional APC were used in our antigen-specific system. The down-regulation of cytokine synthesis in the system of T-T cell presentation could represent a novel mechanism of immune regulation, which may intervene to switch off detrimental Th1- or TM-mediated responses induced by antigen presentation among activated T cells infiltrating inflamed tissues.
Defective Th1 and Th2 cytokine synthesis in the T-T cell presentation model for lack of CD40/CD40 ligand interaction / Lucrezia De, Vita; Accapezzato, Daniele; Mangino, Giorgio; Morrone, Stefania; Isabella, Santilio; Marco Antonio, Casciaro; Danila, Fava; Bruno, Guglielmo; Gianfranco Del, Prete; Santoni, Angela; Barnaba, Vincenzo. - In: EUROPEAN JOURNAL OF IMMUNOLOGY. - ISSN 0014-2980. - 28:11(1998), pp. 3552-3563. [10.1002/(sici)1521-4141(199811)28:11<3552::aid-immu3552>3.0.co;2-x]
Defective Th1 and Th2 cytokine synthesis in the T-T cell presentation model for lack of CD40/CD40 ligand interaction
ACCAPEZZATO, DANIELE;MANGINO, GIORGIO;MORRONE, Stefania;BRUNO, Guglielmo;SANTONI, Angela;BARNABA, Vincenzo
1998
Abstract
In this study, T or NK cell clones used as antigen-presenting cells (T- or NK-APC) were shown to he significantly less efficient than professional APC in inducing Th1 and Th2 cytokines by antigen-specific T cell clones. This phenomenon was not related to a limited engagement of TCR by T-APC, since comparable thresholds of TCR down-regulation were shown when antigen was presented by either T-APC or professional APC. Rather, the stimulatory T-APC weakness was due to their inability, because they are CD40(-), to provide the appropriate co-stimuli to responder T cells both indirectly via IL-12, and partially via direct CD40L triggering on T cells. Indeed, the simultaneous addition of IL-12 and reagents directly engaging CD40L on responder T cells restored T cell cytokine synthesis when antigen was presented by T-APC. In addition, either IL-12 production or blocking of T cell cytokine synthesis by anti-IL-12 p75 antibodies was evident only when professional APC were used in our antigen-specific system. The down-regulation of cytokine synthesis in the system of T-T cell presentation could represent a novel mechanism of immune regulation, which may intervene to switch off detrimental Th1- or TM-mediated responses induced by antigen presentation among activated T cells infiltrating inflamed tissues.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
