CD28-mediated Lck signaling regulates GVHD development and iTreg generation in vivo. BALB/c mice were lethally irradiated (800 cGy) and transplanted with 5 × 106 of TCD-BM cells alone or plus 1 × 106 T cells (CD4+ or CD8+ CD25−) from CD28-WT or CD28-Lck mice. Recipient mice were monitored throughout the experimental period for survival (A) and weight change (B). Using the same BMT setting as in panels A and B, 0.5 × 106 CD8+ cells from normal B6 donors alone or plus 0.5 × 106 CD4+ cells from CD28-WT or CD28-Lck mice were transplanted. Data show recipient survival (C) and weight changes (D) at different days after BMT. (E) BALB/c mice were lethally irradiated (800 cGy) and transplanted with 5 × 106 TCD-BM cells alone or plus 1 × 106 T cells (CD4+CD25−) from CD28-WT and CD28-Lck mice. Two weeks after transplantation, recipient spleens were harvested and measured for expression of surface CD4, CD25, and intercellular Foxp3. Percentage of Tregs (CD25+Foxp3+) on gated donor T cells (H2Kb+CD4+) is shown in each mouse for a total of 3 mice per group, and the data represent 1 of 3 replicate experiments. In separate experiments, CFSE-labeled T cells (CD4+ or CD8+ CD25−) isolated from CD28-WT and CD28-Lck mice were transplanted into lethally irradiated (800 cGy) BALB/c mice at 2 × 106 per mouse. Four days after transplantation, recipient spleens were harvested and measured for CFSE profile, expression of surface CD4 and H2Kb, and intracellular IFNγ. Expression of CD4 and H2Kb was shown on live spleen cells (F). CFSE profile (G) and intracellular IFNγ expression (H) were shown on gated donor CD4 (H2Kb+CD4+) or CD8 (H2Kb+CD4−) T cells. The data represent 1 of 2 replicate experiments.