The sensitivity of IL-4 production for cAMP inducers is lost in CD4+ T cells from aged mice |
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Authors: | Dobber, Ruud van den Bergh, Paula Tielemans, Margret Schuitemaker, Joost Nageikerken, Lex |
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Affiliation: | Section of Immunology, Institute of Aging and Vascular Research TNO PO Box 430, 2300 AK Leiden, The Netherlands |
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Abstract: | CD4+ T cell clones have been demonstrated to display a differentialsensitivity for the induction of cAMP. In the present studywe investigated whether the differential sensitivity of CD4+T cell clones for cAMP inducers is also applicable to freshlyisolated phenotypically and functionally distinct CD4+ T cellsubsets that develop naturally in aging mice. Our results showthat the concanavalin A induced and anti-CD3 induced proliferativeresponse of CD4+ T cells from young mice is more sensitive forprostaglandin E2 (PGE2) and forskolin than that of their agedcounterparts, although the IL-2 production by these cells wasequally sensitive. In contrast, only a slight or no inhibitoryeffect of these cAMP inducers was found when the cells werestimulated with the combination of phorbol myristate acetateand lonomycln. In contrast to the findings obtained with Tn2clones, IL-4 production by freshly isolated CD4+ T cells wasinhibited by the cAMP inducers, whereas exogenous IL-2 had norestorative effect. However, the IL-4 production by CD4+ T cellsfrom aged mice was less sensitive than the IL-4 production byCD4+ T cells from young mice, although CD4+ T cells from agedmice showed significantly higher levels of intracellular cAMPin response to PGE2. These higher levels of cAMP were relatedto the increased fraction of memory cells in aged mice: theMel-14– Pgp-1++ CD4+ T cells responded with at least 2-foldhigher levels of intracellular cAMP than the naive cells inyoung as well as in aged mice. Although memory CD4+ T cellsfrom young as well as aged mice responded vigorously to PGE2by an enhancement of intracellular cAMP, only the IL-4 productionby cells from young mice was significantly inhibited. Therefore,it is not likely that the induction of cAMP is a major eventin the skewing of a primary response towards a Th2 type of response. |
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Keywords: | aging cAMP CD4+ T cells IL-4 memory naive |
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