Figure 6
Figure 6. Local reconstitution of CD8+ DCs inhibits systemic concomitant immunity. Mice were inoculated with B16 cells (105) in the left ear on day 0, and reinoculated with B16 (2.5 × 105) in the right shoulder on day 6. Mice were either untreated (no CTX) of treated with CTX (CTX) 4 days before the primary tumor challenge (A). Mice were treated with CTX as described for panel A and received 106 CD8+ DCs in the left ear 1 day before the primary tumor challenge or were treated with CTX and received 106 CD8− DCs in the left ear using the same timeline (B). The left graphs represent growth of primary tumors, the right graphs depict growth of challenge secondary tumors. P values for the primary tumor were not statistically significant except no CTX and CTX + CD8− DCs (P = .002). P values comparing growth curves between no CTX with CTX, CTX + CD8+ DCs, and CTX + CD8− CCs were < .001, .031, and < .001, respectively. The P value comparing CTX versus CTX + CD8+ DCs was .004. The growth of the second challenge tumor inoculum in naive mice without primary tumor challenge (with or without CTX treatment; C). Data from 1 of 2 independent experiments with similar results are shown.

Local reconstitution of CD8+ DCs inhibits systemic concomitant immunity. Mice were inoculated with B16 cells (105) in the left ear on day 0, and reinoculated with B16 (2.5 × 105) in the right shoulder on day 6. Mice were either untreated (no CTX) of treated with CTX (CTX) 4 days before the primary tumor challenge (A). Mice were treated with CTX as described for panel A and received 106 CD8+ DCs in the left ear 1 day before the primary tumor challenge or were treated with CTX and received 106 CD8 DCs in the left ear using the same timeline (B). The left graphs represent growth of primary tumors, the right graphs depict growth of challenge secondary tumors. P values for the primary tumor were not statistically significant except no CTX and CTX + CD8 DCs (P = .002). P values comparing growth curves between no CTX with CTX, CTX + CD8+ DCs, and CTX + CD8 CCs were < .001, .031, and < .001, respectively. The P value comparing CTX versus CTX + CD8+ DCs was .004. The growth of the second challenge tumor inoculum in naive mice without primary tumor challenge (with or without CTX treatment; C). Data from 1 of 2 independent experiments with similar results are shown.

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