Immunomodulation
Excessive CpG 1668 stimulation triggers IL-10 production by cDC that inhibits IFN-α responses by pDC
Article first published online: 7 NOV 2008
DOI: 10.1002/eji.200838184
Copyright © 2008 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim
Additional Information
How to Cite
Waibler, Z., Anzaghe, M., Konur, A., Akira, S., Müller, W. and Kalinke, U. (2008), Excessive CpG 1668 stimulation triggers IL-10 production by cDC that inhibits IFN-α responses by pDC. Eur. J. Immunol., 38: 3127–3137. doi: 10.1002/eji.200838184
Publication History
- Issue published online: 7 NOV 2008
- Article first published online: 7 NOV 2008
- Manuscript Accepted: 26 AUG 2008
- Manuscript Revised: 25 JUL 2008
- Manuscript Received: 28 JAN 2008
Funded by
- Deutsche Forschungsgemeinschaft. Grant Numbers: SFB432, B15
- EU INVADERS. Grant Number: QLK2-CT-2001-02103
- ZAFES (CpG-Cluster)
Keywords:
- Autoimmunity;
- DC;
- Type I IFN
Abstract
Upon stimulation with a wide range of concentrations of CpG oligodeoxynucleotide 2216 (CpG 2216), plasmacytoid DC are induced to produce type I IFN (IFN-α/β). In contrast, CpG 1668 shows a bell-shaped dose–response correlation, i.e. only intermediate but not high doses of CpG 1668 induce IFN-α/β. Interestingly, high-dose CpG 1668 completely inhibited IFN-α responses induced by CpG 2216. Experiments using supernatant of high-dose CpG-1668-treated cells indicated that secreted inhibitor(s) mediated the IFN-α shut-off. Among modulating cytokines, IL-10 turned out to be one important negative regulator. In line with this, supernatants of IL-10-deficient DC cultures stimulated with high-dose CpG 1668 did not inhibit IFN-α production. Interestingly, high-dose CpG 1668 also inhibited IFN-α responses induced by the DNA-encoded mouse cytomegalovirus, whereas IFN-α responses induced by negative-strand RNA-encoded vesicular stomatitis virus were only marginally affected. Experiments with DC cultures devoid of TLR9 indicated that TLR9 was critically required to mediate stimulatory and modulatory signals by low and high concentrations of CpG 1668, respectively. Analysis of purified DC subsets showed that conventional DC were the main IL-10 producers, whereas plasmacytoid DC hardly produced any IL-10.

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