Figure 1
Figure 1. Loss of bad or bmf accelerates c-myc–induced lymphomagenesis. (A) Tumor-free survival of Eμ-myc (n = 29; median survival, 138 days), Eμ-myc/bad+/− (n = 47; median survival, 100 days), Eμ-myc/bad−/− (n = 29; median survival, 78 days), and Eμ-myc/bim+/− (n = 32; median survival, 67 days). Lymphomas occurred significantly earlier in Eμ-myc/bad−/− than in wt Eμ-myc animals (P < .001). (B) Tumor-free survival of Eμ-myc, Eμ-myc/bmf+/− (n = 30; median survival, 100 days), Eμ-myc/bmf−/− (n = 30; median survival, 87 days), and Eμ-myc/bim+/−. Lymphomas occurred significantly earlier in Eμ-myc/bmf+/− (P < .05) and Eμ-myc/bmf−/− (P < .01) than in wt Eμ-myc animals. (C) Tumor -free survival of Eμ-myc/bad−/−bmf+/+, Eμ-myc/bad−/−bmf+/− (n = 16), and Eμ-myc/bad−/−bmf−/− mice (n = 11). (D) Distributions of pro/pre-B (light gray), mixed (dark gray), IgM+ (black), and B220+CD4+ (white) lymphomas occurring in mice of the indicated genotypes. The distribution of lymphoma phenotypes was significantly different in Eμ-myc/bmf−/− compared with Eμ-myc animals (P < .01, χ2 test). (E) Kaplan-Meier analysis of IgM+ and mixed lymphomas (top) and of pre-B lymphomas (bottom) of Eμ-myc (black solid line), Eμ-myc/bad+/− (light gray, dashed line), Eμ-myc/bad−/− (light gray, solid line), Eμ-myc/bmf+/− (dark gray dotted line), and Eμ-myc/bmf−/− (dark gray solid line) mice. IgM+ B lymphomas arose significantly earlier in Eμ-myc/bmf−/− (P < .001) and Eμ-myc/bad−/− (P < .01) than in wt Eμ-myc mice. Pre-B lymphomas were not significantly accelerated by loss of either bad or bmf.

Loss of bad or bmf accelerates c-myc–induced lymphomagenesis. (A) Tumor-free survival of Eμ-myc (n = 29; median survival, 138 days), Eμ-myc/bad+/− (n = 47; median survival, 100 days), Eμ-myc/bad−/− (n = 29; median survival, 78 days), and Eμ-myc/bim+/− (n = 32; median survival, 67 days). Lymphomas occurred significantly earlier in Eμ-myc/bad−/− than in wt Eμ-myc animals (P < .001). (B) Tumor-free survival of Eμ-myc, Eμ-myc/bmf+/− (n = 30; median survival, 100 days), Eμ-myc/bmf−/− (n = 30; median survival, 87 days), and Eμ-myc/bim+/−. Lymphomas occurred significantly earlier in Eμ-myc/bmf+/− (P < .05) and Eμ-myc/bmf−/− (P < .01) than in wt Eμ-myc animals. (C) Tumor -free survival of Eμ-myc/bad−/−bmf+/+, Eμ-myc/bad−/−bmf+/− (n = 16), and Eμ-myc/bad−/−bmf−/−mice (n = 11). (D) Distributions of pro/pre-B (light gray), mixed (dark gray), IgM+ (black), and B220+CD4+ (white) lymphomas occurring in mice of the indicated genotypes. The distribution of lymphoma phenotypes was significantly different in Eμ-myc/bmf−/− compared with Eμ-myc animals (P < .01, χ2 test). (E) Kaplan-Meier analysis of IgM+ and mixed lymphomas (top) and of pre-B lymphomas (bottom) of Eμ-myc (black solid line), Eμ-myc/bad+/− (light gray, dashed line), Eμ-myc/bad−/− (light gray, solid line), Eμ-myc/bmf+/− (dark gray dotted line), and Eμ-myc/bmf−/− (dark gray solid line) mice. IgM+ B lymphomas arose significantly earlier in Eμ-myc/bmf−/− (P < .001) and Eμ-myc/bad−/− (P < .01) than in wt Eμ-myc mice. Pre-B lymphomas were not significantly accelerated by loss of either bad or bmf.

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