Abstract
Following positive selection, NKT cell precursors enter an “NK-like” program and progress from an NK– to an NK+ maturational stage to give rise to NKT1 cells. Maturation takes place in the thymus or after emigration of NK– NKT cells to the periphery. In this study, we followed the fate of injected NKT cells at the NK– stage of their development in the thymus of a series of mice with differential CD1d expression. Our results indicate that CD1d-expressing cortical thymocytes, and not epithelial cells, macrophages, or dendritic cells, are necessary and sufficient to promote the maturation of thymic NKT1 cells. Migration out of the thymus of NK– NKT cells occurred in the absence of CD1d expression, however, CD1d expression is required for maturation in peripheral organs. We also found that the natural ligand Isoglobotriosylceramide (iGb3), and the cysteine protease Cathepsin L, both localizing with CD1d in the endosomal compartment and crucial for NKT cell positive selection, are also required for NK– to NK+ NKT cell transition. Overall, our study indicates that the maturational transition of NKT cells require continuous TCR/CD1d interactions and suggest that these interactions occur in the thymic cortex where DP cortical thymocytes are located. We thus concluded that key components necessary for positive selection of NKT cells are also required for subsequent maturation.
Highlights
Mouse NKT cells are the product of a special developmental program initiated after their encounter with CD1d molecules presenting self-lipid antigens in the thymus
We show that thymic transition of NKT cells from the NK− to the NK+ stage does not require CD1d expression on specialized APC or on epithelial cells, but that cortical thymocytes play a crucial role by presenting the natural ligand to NKT cells
We found that CD1d expression on cortical thymocytes, but not APC or epithelial cells, is required to drive maturation of already selected NKT1 cells; and that this maturation step is not required for NKT cells to migrate from the thymus to the periphery
Summary
Mouse NKT cells are the product of a special developmental program initiated after their encounter with CD1d molecules presenting self-lipid antigens in the thymus. Mouse NKT cells were first described as expressing a semi-invariant Vα14-Jα18/Vβ8,Vβ7,Vβ2 αβ T cell receptor (Vα14-Jα18/Vβ TCR) and NK-lineage markers, such as receptors belonging to the CD94/NKG2 or LY49 families [2]. In a few mouse strains such as C57BL/6 where NKT cells have been initially extensively studied, they express the NK1.1 receptor. NKT cells express the activation marker CD44 and have functional features of NK cells, producing IFN-γ upon stimulation. These cells are fully mature and are at an end, or stage 3, developmental stage
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