Figure 1.
ICOS expression is up-regulated upon alloactivation and during GVHD. (A) In vivo–alloactivated T cells up-regulate ICOS expression. B6 splenocytes were labeled with CFSE and transferred into a sublethally irradiated (750 cGy) syngeneic B6 or allogeneic C3FeB6F1 recipients. Transferred cells were analyzed after 72 hours for ICOS expression. A horizontal line represents the fluorescence intensity of negative controls for both isotype-stained and unstained cells. T cells were stained for donor T-cell origin and were analyzed by gating on Ly9.1-, CD3+, and CD4+, or CD8+. Data from 1 mouse is representative of 2 independent experiments (n = 3 per experiment). (B) ICOS is highly expressed on alloreactive T cells during GVHD. C3FeB6F1 mice were lethally irradiated (1300 cGy split) and received transplants with TCD allo-HSCs and 1 × 106 T cells from B6 mice. Donor T cells were harvested from recipients' spleens 7 and 14 days after transplantation (GVHD day 7, day 14) and analyzed for ICOS cell surface expression in CD44hi cells. As controls, splenocytes from B6 mice not receiving transplants were used (control), and insets show CD44 subpopulations. Gray histograms represent the isotype control, and the black histograms represent staining with anti-ICOS monoclonal antibody. Shown are representative data of 1 mouse each from 1 independent experiment (normal mouse and day 7, n = 5) and 2 independent experiments (day 14, n = 5 to 8).