Fig. 2. Inhibition of the NF-κB pathway abolished CD8⁺ T cell–mediated NKG2D ligand upregulation.

CT26 (A) and K7M3 (B) cells were pretreated with an NF-κB pathway inhibitor: STAT inhibitor S3I-201 (50 μM for 24 h), p38 inhibitor PH797804 (1 μM for 4 h), MAPK kinase (MEK) inhibitor PD98059 (2 μM for 4 h), PI3K inhibitor PKI-587 (5 nM for 4 h), or NF-κB inhibitor QNZ (100 nM for 4 h). The pretreated cells were then labeled with CFSE and cultured in the presence or absence of stimulated mouse CD8⁺ T cells (1:1 tumor cell-to-T cell ratio). Rae-1 expression on the tumor cell surface was determined via flow cytometry. iso ctrl: isotype control. Bar graphs show means ± SEM. Results are representative of three repeated experiments. ** P<0.01; **** P<0.001; ns, no statistical significance