JCI - Fanconi anemia pathway–deficient tumor cells are hypersensitive to inhibition of ataxia telangiectasia mutated

Fanconi anemia pathway–deficient tumor cells are hypersensitive to inhibition of ataxia telangiectasia mutated

Richard D. Kennedy, Clark C. Chen, Patricia Stuckert, Elyse M. Archila, Michelle A. De la Vega, Lisa A. Moreau, Akiko Shimamura, Alan D. D’Andrea

Published in Volume 117, Issue 5

J Clin Invest. 2007; 117(5):1440–1449 doi:10.1172/JCI31245

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Figure 6

The FA pathway–deficient HS766T pancreatic cancer cell line is sensitive to KU-55933.

(A) A clonogenic assay comparing the number of colonies in FANCG mutant HS766T cells (black bars) and the isogenic FANCG-corrected cell line (white bars) 14 days after KU-55933 treatment. Bars 1 and 2 represent untreated controls. Bars 3 and 4 represent cells treated with 5 μM KU-55933. Bars 5 and 6 represent cells treated with 10 μM KU-55933. Colony counts are shown as a percentage of the untreated control for each cell line. (B) A clonogenic assay comparing the number of colonies in FANCC mutant PL11 cells (black bars) and the isogenic FANCC-corrected cell line (white bars) 14 days after KU-55933 treatment. Bars 1 and 2 represent untreated controls. Bars 3 and 4 represent cells treated with 5 μM KU-55933. Bars 5 and 6 represent cells treated with 10 μM KU-55933. Colony counts are shown as a percentage of the untreated control for each cell line. (C) A Western blot comparing FANCD2 monoubiquitination and ATM autophosphorylation in the FANCG mutant HS766T cell line (lanes 1 and 3) and the isogenic FANCG-corrected cell line (lanes 2 and 4). Lanes 1 and 2 represent an untreated control. Lanes 3 and 4 represent cells treated for 24 hours with 10 μM KU-55933. The upper band in the FANCG blot is a nonspecific cross-reacting band.