Figure 2
Figure 2. TGFβ signaling is required for RORγt+ iNKT development. (A) Flow cytometry analysis of the presence of iNKT cell subsets in the thymus and pLNs of CD4-Cre; TgfbRIIflox/flox mice (TGFβRII°) and WT littermate control. Mice were analyzed at 2 weeks old, before the onset of T cell–mediated autoimmunity.22,41 (B) Mean absolute numbers ± SEM of CD4− RORγt+ and conventional RORγt− iNKT cells from the thymus and pLNs. (C) Flow cytometry analysis of the expression of RORγt in CD4 single-positive (CD4 SP), DP, and total iNKT cells (iNKT) in the thymus. Invariant NKT cells were identified by excluding B220+ and CD8+ cells and gating on CD1d tetramer+ TCRβ+ cells. Representative plots and combined data of 6 experiments totaling 8 to 10 mice in each group. P values were calculated using an unpaired Student t test (*P < .05; **P < .01; ***P < .001).

TGFβ signaling is required for RORγt+ iNKT development. (A) Flow cytometry analysis of the presence of iNKT cell subsets in the thymus and pLNs of CD4-Cre; TgfbRIIflox/flox mice (TGFβRII°) and WT littermate control. Mice were analyzed at 2 weeks old, before the onset of T cell–mediated autoimmunity.22,41  (B) Mean absolute numbers ± SEM of CD4 RORγt+ and conventional RORγt iNKT cells from the thymus and pLNs. (C) Flow cytometry analysis of the expression of RORγt in CD4 single-positive (CD4 SP), DP, and total iNKT cells (iNKT) in the thymus. Invariant NKT cells were identified by excluding B220+ and CD8+ cells and gating on CD1d tetramer+ TCRβ+ cells. Representative plots and combined data of 6 experiments totaling 8 to 10 mice in each group. P values were calculated using an unpaired Student t test (*P < .05; **P < .01; ***P < .001).

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