Figure 6
Figure 6. GVHD and GVL responses are enhanced by type I-IFN signaling in donor grafts. (A) Survival and clinical scores in lethally irradiated B6D2F1 mice transplanted with 5 × 106 BM and 2 × 106 T cells from either B6.WT or B6.IFNAR1−/− donors (#P < .005, **P < .01, *P < .05; combined data from 3 experiments, n = 26-30 in BM + T groups, n = 13 in TCD controls). (B) Leukemic death after administration of host derived P815luc+ tumor (5 × 103) with the donor graft (*P < .05, B6.WT vs B6.IFNAR1−/− donors; combined data from 2 experiments, n = 18 in BM + T groups, n = 8 in TCD control groups). (C) Bioluminescence at day 12 after transplantation with P815luc+ tumor (**P < .01, B6.WT vs B6.IFNAR1−/− donors; combined data from 2 experiments, n = 18 per gp) with representative images shown. (D) In vivo cytotoxicity index at day 12 after BM transplantation (data combined from 2 experiments and expressed as mean ± SEM; *P < .05, B6.WT vs B6.IFNAR1−/− donors, n = 7-11 per group). (E) Leukemic death after transplantation of lethally irradiated B6D2F1 mice with a combination of either B6.WT or B6.IFNAR1−/− BM with B6.WT or B6.IFNAR1−/− T cells and P815luc+ tumor (**P < .01, *P < .05, combined data from 2 experiments, n = 16 in BM + T groups, n = 8 in TCD). (F) B6.WT recipients were lethally irradiated and 24 hours later 107 BM and 106 CD8+ T cells from C3H.SW donors transplanted with 2.5 × 104 EL-4luc+ tumor. After the establishment of low-level tumor as determined by bioluminescence, recombinant IFNα or saline was administered every other day and tumor burden assessed 1 week later (data combined from 2 experiments and expressed as mean ± SEM; **P < .01 saline day 0 vs day 7).

GVHD and GVL responses are enhanced by type I-IFN signaling in donor grafts. (A) Survival and clinical scores in lethally irradiated B6D2F1 mice transplanted with 5 × 106 BM and 2 × 106 T cells from either B6.WT or B6.IFNAR1−/− donors (#P < .005, **P < .01, *P < .05; combined data from 3 experiments, n = 26-30 in BM + T groups, n = 13 in TCD controls). (B) Leukemic death after administration of host derived P815luc+ tumor (5 × 103) with the donor graft (*P < .05, B6.WT vs B6.IFNAR1−/− donors; combined data from 2 experiments, n = 18 in BM + T groups, n = 8 in TCD control groups). (C) Bioluminescence at day 12 after transplantation with P815luc+ tumor (**P < .01, B6.WT vs B6.IFNAR1−/− donors; combined data from 2 experiments, n = 18 per gp) with representative images shown. (D) In vivo cytotoxicity index at day 12 after BM transplantation (data combined from 2 experiments and expressed as mean ± SEM; *P < .05, B6.WT vs B6.IFNAR1−/− donors, n = 7-11 per group). (E) Leukemic death after transplantation of lethally irradiated B6D2F1 mice with a combination of either B6.WT or B6.IFNAR1−/− BM with B6.WT or B6.IFNAR1−/− T cells and P815luc+ tumor (**P < .01, *P < .05, combined data from 2 experiments, n = 16 in BM + T groups, n = 8 in TCD). (F) B6.WT recipients were lethally irradiated and 24 hours later 107 BM and 106 CD8+ T cells from C3H.SW donors transplanted with 2.5 × 104 EL-4luc+ tumor. After the establishment of low-level tumor as determined by bioluminescence, recombinant IFNα or saline was administered every other day and tumor burden assessed 1 week later (data combined from 2 experiments and expressed as mean ± SEM; **P < .01 saline day 0 vs day 7).

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