Figure 2
Figure 2. LICs lacking the cytokine receptor γC exhibit increased sensitivity to dasatinib therapy in vivo. (A) Mice infused with the indicated numbers of γC-positive LICs (i) or γC-null LICs (ii-iv) were imaged for vector luciferase activity 10 days later. Matched exposures document relative levels of fluorescence radiance indicated at the right. (B) Cohorts of mice receiving 2 × 105 γC -positive LICs (Ai) or 2 × 106 γC -null LICs (Aiii) were left untreated or were treated once daily 5 days per week with vehicle or dasatinib (10 mg/kg body weight) and euthanized when moribund. Despite their more significant leukemia burden at day 10 (Aiii vs Ai), mice receiving γC-null LICs exhibited a better response to dasatinib therapy. Statistics for pairwise comparisons: untreated vs vehicle (whether γC WT or null groups) are not significant; γC WT, vehicle vs dasatinib, P < .001; γC null, vehicle vs dasatinib, P < .001; dasatinib-treated γC WT vs dasatinib-treated γC null, P = .014. Rx, treatment; WT, wild-type.

LICs lacking the cytokine receptor γC exhibit increased sensitivity to dasatinib therapy in vivo. (A) Mice infused with the indicated numbers of γC-positive LICs (i) or γC-null LICs (ii-iv) were imaged for vector luciferase activity 10 days later. Matched exposures document relative levels of fluorescence radiance indicated at the right. (B) Cohorts of mice receiving 2 × 105 γC -positive LICs (Ai) or 2 × 106 γC -null LICs (Aiii) were left untreated or were treated once daily 5 days per week with vehicle or dasatinib (10 mg/kg body weight) and euthanized when moribund. Despite their more significant leukemia burden at day 10 (Aiii vs Ai), mice receiving γC-null LICs exhibited a better response to dasatinib therapy. Statistics for pairwise comparisons: untreated vs vehicle (whether γC WT or null groups) are not significant; γC WT, vehicle vs dasatinib, P < .001; γC null, vehicle vs dasatinib, P < .001; dasatinib-treated γC WT vs dasatinib-treated γC null, P = .014. Rx, treatment; WT, wild-type.

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