Indentification Of Novel Ligands That Alter The Function Of Type Ii Nkt Cells

Abstract Natural killer T (NKT) cells are distinct innate lymphocytes which recognize lipid antigens in the context of the major histocompatibility complex-like molecule CD1d. When activated, these cells can rapidly produce a variety of cytokines and modulate innate and adaptive immune responses. There are two main subsets of NKT cells, termed type I and type II NKT cells. Type I NKT cells are characterized primarily on the basis of their invariant TCRα expression and reactivity to the glycolipid α-galactosyl ceramide (αGalCer), whereas type II NKT cells express a different and more diverse TCR repertoire than type I NKT cells. Currently, the most widely studied antigen for type II NKT cells is sulfatide. Sulfatide-reactive type II NKT cells are reported to have the immunosuppressive function in autoimmune diseases and cancer. We previously showed a role for sulfatide-reactive type II NKT cells in suppressing tumor immunosurveillance in a murine model of lung metastasis. The activation of type II NKT cells in this model by the injection of sulfatide increased the development of lung metastasis. We synthesized diverse sulfatide-analogues varying in the number of double bonds and hydroxyl groups in the ceramide. In vitro, analogues having a phytosphingosine sphingoid base activated both type II and type I NKT cell hybridomas. On the other hand, the analogue C24:2 with a sphingosine base activated only the type II NKT cell hybridoma. In vivo, the C24:2 analogue significantly reduced the development of lung metastasis, showing distinct and opposite effects from sulfatide. The identification of new ligands inducing altered functional activity of type II NKT cells could be of great interest for developing new anti-tumor immunotherapies.