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Mark Y. Chiang, Lanwei Xu, Olga Shestova, Gavin Histen, Sarah L’Heureux, Candice Romany, M. Eden Childs, Phyllis A. Gimotty, Jon C. Aster, Warren S. Pear
Published in Volume 118, Issue 9
J Clin Invest. 2008; 118(9):3181–3194 doi:10.1172/JCI35090
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Figure 5
Notch1 GOF allele strength and T-ALL induction.

Lethally irradiated mice were reconstituted with 5-FU–treated donor BM cells that were transduced with the indicated Notch1 alleles. Kaplan-Meier graphs show the fraction of mice without T-ALL as a function of time. Only tumors having intact proviral integrants were included in the analysis. MigR1 and ICN1 mice were negative and positive controls, respectively, that were compared with L1601P and L1601PΔP (A); L1594P and L1594PΔP (B); N1ΔP (C); and P12 and P12ΔP (D). Individual cohorts contained 6–12 mice transduced with each allele, and each experiment was performed at least twice. Representative tissue sections showing Notch-associated T-ALLs infiltrating the liver (H&E stain) are shown in E and F. Original magnification, ×400.