Abstract
The qualitative nature of immune responses induced by dendritic cells (DCs) is influenced by the balance of pro-inflammatory (e.g. IL-12) and anti-inflammatory (e.g. IL-10) cytokines that they secrete. Evidence to date suggests that IL-12 and IL-10 secretion is reciprocally regulated and that IL-10 inhibits IL-12 secretion. This study identifies a population of resting, immature rat bone marrow-derived DCs (BMDCs) which secretes IL-10, the IL-12 p70 heterodimer and the free IL-12 p40 subunit, the latter in vast excess of IL-12 p70. Counter-intuitively, activation with LPS induces the secretion of high and equivalent levels of IL-10 and IL-12 p40, but only quantitatively small increases in IL-12 p70. Neutralization of IL-10 increased the secretion of IL-12 p40 by resting BMDCs, but decreased IL-12 p40 secretion by LPS-activated BMDCs. Pre-incubation of resting BMDCs for 24 h with neutralizing antibody to IL-10 reduced the subsequent secretion of IL-10 in allogeneic cultures of Lewis CD3 + T cells with resting and LPS-activated Wistar BMDCs, and enhanced IL-12 p40 secretion in allogeneic cultures with LPS-activated BMDCs. IL-10 neutralization had no effect on the levels of IL-12 p70, IFN- γ or IL-4 in allogeneic cultures. In summary, this study has identified a population of rat BMDCs that secretes low levels of bioactive IL-12 p70, but high levels of IL-10 and IL-12 p40. These findings argue against the concept that there is a reciprocal relationship between IL-10 and IL-12 secretion. They might also have implications for understanding the role of DCs in post-activation qualitative skewing of immune responses.
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