Figure 3
Immunization with allogeneic CD8α+ DCs reduces T-cell–proliferative response without altering their rate of apoptosis. T cells were harvested from BALB/c mice that were immunized with diluent or B6 BM-derived CD8α+ DC and CD8α− DC subsets as described in “Methods.” BALB/c CD90+ T cells (2 × 106/well) were then stained with CFSE and stimulated in vitro with B6 BM DCs for 96 hours and analyzed by flow cytometry. (A) Gated for fluorescein isothiocynate–conjugated CFSE and allophycocyanin-conjugated CD3+ T cells. Data are representative of 1 of 4 independent similar experiments. Combined data for the nonimmunized, CD8α+ DC–vaccinated, and CD8α− DC–vaccinated are 0.77% ± 0.15%, 24.1% ± 2.4%, 4.7% ± 1.6%, and 18.1% ± 0.6%, respectively (P < .04, nonimmunized vs CD8α+ DC). (B) PE-conjugated annexin V and allophycocyanin-conjugated anti-CD3. P = not significant between the groups. Data are representative of 1 of 3 independent similar experiments.

Immunization with allogeneic CD8α+ DCs reduces T-cell–proliferative response without altering their rate of apoptosis. T cells were harvested from BALB/c mice that were immunized with diluent or B6 BM-derived CD8α+ DC and CD8α DC subsets as described in “Methods.” BALB/c CD90+ T cells (2 × 106/well) were then stained with CFSE and stimulated in vitro with B6 BM DCs for 96 hours and analyzed by flow cytometry. (A) Gated for fluorescein isothiocynate–conjugated CFSE and allophycocyanin-conjugated CD3+ T cells. Data are representative of 1 of 4 independent similar experiments. Combined data for the nonimmunized, CD8α+ DC–vaccinated, and CD8α DC–vaccinated are 0.77% ± 0.15%, 24.1% ± 2.4%, 4.7% ± 1.6%, and 18.1% ± 0.6%, respectively (P < .04, nonimmunized vs CD8α+ DC). (B) PE-conjugated annexin V and allophycocyanin-conjugated anti-CD3. P = not significant between the groups. Data are representative of 1 of 3 independent similar experiments.

Close Modal
This Feature Is Available To Subscribers Only

or Create an Account

Close Modal
Close Modal