EAE was induced in SJL mice by transfer of encephalitogenic T cells from donor mice to recipient mice. (A and B) Donor mice received 3 consecutive ECS (n = 7) or sham (control, n = 7) treatments on days 8–10 p.i. Twenty-four hours later, lymph node cells were isolated from ECS-treated or the control group and injected into 2 groups of naive mice (day 0). Disease severity and pattern were similar between the 2 recipient groups. Data represent mean ± SD (A). No significant difference was found in the cumulative score between the mice that received encephalitogenic lymphocytes from the control or the ECS-treated group (B). The experiment was repeated twice. (C and D) Encephalitogenic lymphocytes from control or ECS-treated mice were activated in vitro with PLP or ConA. Representative FACS image (from 3 independent experiments) of Brdu⁺ cells showing similar percentage of proliferating cells from ECS and sham-treated donor mice in response to PLP (C). FACS analysis of Brdu-stained cells showed no significant difference in the percentage of Brdu⁺ cells between the groups when not activated (naive) or activated with PLP (quantification of C) or ConA (D). Three independent experiments were performed. Data represent mean ± SEM. (E and F) Recipient mice treated with 3 consecutive ECS (n = 10 mice) or sham (n = 11 mice) treatments, starting at day 8 after transfer, upon first presentation of clinical signs. Disease severity and length was reduced among the ECS-treated group. Data represent mean ± SD (E). Cumulative score was significantly reduced in the recipient mice treated with ECS (F). The experiment was repeated twice. Box-and-whisker plots show quartiles with median, and with minima and maxima at the bottom and top whiskers, respectively. P values calculated with Student’s unpaired t test.