The pro-Th2 cytokine IL-33 directly interacts with invariant NKT and NK cells to induce IFN-gamma production
- Authors
- Type
- Published Article
- Journal
- European Journal of Immunology
- Publisher
- Wiley (John Wiley & Sons)
- Publication Date
- Apr 06, 2009
- Volume
- 39
- Issue
- 4
- Pages
- 1046–1055
- Identifiers
- DOI: 10.1002/eji.200838575
- PMID: 19266498
- Source
- MyScienceWork
- Keywords
- License
- Green
Abstract
IL-33 has recently been identified as a cytokine endowed with pro-Th2 functions, raising the question of its effect on invariant natural killer T cell (iNKT), which are potent IL-4 producers. Here, we report a two-fold increase of iNKT-cell counts in spleen and liver after a 7-day treatment of mice with IL-33, which results from a direct effect, given that purified iNKT cells express the T1/ST2 receptor constitutively and respond to IL-33 by in vitro expansion and functional activation. Conversely to the expected pro-Th2 effect, IL-33 induced a preferential increase in IFN-gamma rather than IL-4 production upon TCR engagement that depended on endogenous IL-12. Moreover, in combination with the pro-inflammatory cytokine IL-12, IL-33 enhanced IFN-gamma production by both iNKT and NK cells. Taken together these data support the conclusion that IL-33 can contribute as a co-stimulatory factor to innate cellular immune responses.