IL-2 triggers specific signaling pathways in human NKT cells leading to the production of pro- and anti-inflammatory cytokines

Stéphanie Bessoles^*, Frédéric Fouret^*, Sherri Dudal^*, Gurdyal S. Besra, Françoise Sanchez^* and Virginie Lafont^*^,1

^* Université Montpellier 1, Centre d’étude d’agents Pathogènes et Biotechnologies pour la Santé, CNRS UMR 5236, Montpellier, France; and
School of Biosciences, University of Birmingham, Edgbaston, Birmingham, United Kingdom

¹Correspondence: UMR 5236, Université de Montpellier II, Place Eugene Bataillon, CC 100, 34095 Montpellier Cedex 05, France. E-mail: vlafont{at}crit.univ-montp2.fr

NKT cells belong to a conserved T lymphocyte subgroup that hasbeen implicated in the regulation of various immune responses,including responses to viruses, bacteria, and parasites. Theyexpress a semi-invariant TCR that recognizes glycolipids presentedby the nonpolymorphic MHC class I-like molecule CD1d, and uponactivation, they produce various pro- and anti-inflammatorycytokines. Recent studies have shed light on the nature of glycolipidsand the environmental signals that may influence the productionof cytokines by NKT cells and thus, modulate the immune response.To better understand the regulation mechanisms of NKT cells,we explored their behavior following activation by IL-2 andinvestigated the signaling pathways and biological responsestriggered. We demonstrated that IL-2 activates not only STAT3and -5 and the PI-3K and ERK-2 pathways as in all IL-2 respondercells but also STAT4 as in NK cells and the p38 MAPK pathwayas in ${alpha}$ β T cells. We also showed that STAT6 is activatedby IL-2 in NKT cells. Moreover, IL-2 induces the productionof IFN- ${gamma}$ and IL-4. The ability of IL-2 to induce pro- and anti-inflammatorycytokine production, in addition to proliferation, could opennew therapeutic approaches for use in combination with moleculesthat activate NKT cells through TCR activation.

Key Words: nonconventional lymphocytes • STAT