Fig. 6.
Fig. 6. Effect of blockade of the OX40/OX40L pathway on GVHD lethality in settings in which CD28 signaling is precluded. / Blockade of the OX40/OX40L pathway is effective in inhibiting GVHD lethality in settings in which CD28 signaling is precluded. (A-B) B10.BR recipients (n = 8 per group) were lethally irradiated and reconstituted with B6 BM, and cohorts were given C28−/−splenocytes at 15 × 106 (panel A) or 25 × 106 (panel B). Recipients given splenocytes also received either irrelevant, anti-OX40, or anti-OX40L mAb. Survival was significantly different in groups receiving irrelevant mAb versus groups receiving either anti-OX40 or anti-OX40L mAb. (C) BALB/c OX40L−/− mice or OX40L+/+littermate controls (n = 5 per group) were lethally irradiated, reconstituted with B6 WT BM, and given either no T cells or B6 CD28−/− T cells (3 × 106). OX40L−/− recipients had a significantly higher survival rate than OX40L+/+ recipients.

Effect of blockade of the OX40/OX40L pathway on GVHD lethality in settings in which CD28 signaling is precluded.

Blockade of the OX40/OX40L pathway is effective in inhibiting GVHD lethality in settings in which CD28 signaling is precluded. (A-B) B10.BR recipients (n = 8 per group) were lethally irradiated and reconstituted with B6 BM, and cohorts were given C28−/−splenocytes at 15 × 106 (panel A) or 25 × 106 (panel B). Recipients given splenocytes also received either irrelevant, anti-OX40, or anti-OX40L mAb. Survival was significantly different in groups receiving irrelevant mAb versus groups receiving either anti-OX40 or anti-OX40L mAb. (C) BALB/c OX40L−/− mice or OX40L+/+littermate controls (n = 5 per group) were lethally irradiated, reconstituted with B6 WT BM, and given either no T cells or B6 CD28−/− T cells (3 × 106). OX40L−/− recipients had a significantly higher survival rate than OX40L+/+ recipients.

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