Treatment of B-RAF mutant human tumor cells with a MEK inhibitor requires Bim and is enhanced by a BH3 mimetic
Mark S. Cragg, … , Andreas Strasser, Clare L. Scott
Mark S. Cragg, … , Andreas Strasser, Clare L. Scott
Published October 23, 2008
Citation Information: J Clin Invest. 2008;118(11):3651-3659. https://doi.org/10.1172/JCI35437.
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Research Article

Treatment of B-RAF mutant human tumor cells with a MEK inhibitor requires Bim and is enhanced by a BH3 mimetic

Abstract

B-RAF is frequently mutated in solid tumors, resulting in activation of the MEK/ERK signaling pathway and ultimately tumor cell growth and survival. MEK inhibition in these cells results in cell cycle arrest and cytostasis. Here, we have shown that MEK inhibition also triggers limited apoptosis of human tumor cell lines with B-RAF mutations and that this effect was dependent on upregulation and dephosphorylation of the proapoptotic, Bcl-2 homology 3–only (BH3-only) Bcl-2 family member Bim. However, upregulation of Bim was insufficient for extensive apoptosis and was countered by overexpression of Bcl-2. To overcome apoptotic resistance, we treated the B-RAF mutant cells both with MEK inhibitors and with the BH3 mimetic ABT-737, resulting in profound synergism and extensive tumor cell death. This treatment was successful because of both efficient antagonism of the prosurvival Bcl-2 family member Mcl-1 by Bim and inhibition of Bcl-2 and Bcl-xL by ABT-737. Critically, addition of ABT-737 converted the predominantly cytostatic effect of MEK inhibition to a cytotoxic effect, causing long-term tumor regression in mice xenografted with human tumor cell lines. Thus, the therapeutic efficacy of MEK inhibition requires concurrent unleashing of apoptosis by a BH3 mimetic and represents a potent combination treatment for tumors harboring B-RAF mutations.

Authors

Mark S. Cragg, Elisa S. Jansen, Michele Cook, Claire Harris, Andreas Strasser, Clare L. Scott

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Figure 3

MEK inhibition–induced apoptosis of B-RAF mutant tumor cells can be inhibited by Bim KD or Bcl-2 overexpression.

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MEK inhibition–induced apoptosis of B-RAF mutant tumor cells can be inhi...
(A) Top: Western blot analysis documents the levels of Bim and β-actin (loading control) expression in parental and 2 independent RNAi Bim KD subclones of Colo205 cells. Bottom: Parental and RNAi Bim KD subclone 18 Colo205 cells were not treated or were treated for 6 or 24 h with 20 μM UO126 and analyzed by Western blotting for their levels of Bim. (B) Parental, Bim RNAi KD, and Bcl-2–overexpressing clones of Colo205 cells were treated for 48 h with 0–40 μM UO126 as indicated, and cell survival was examined by FACS analysis. Data (mean ± SD of 3 or 4 independent clones) indicate percent cell death relative to untreated cells. (C) Clonogenic survival assays of parental, Bim RNAi KD, and Bcl-2–overexpressing clones of Colo205 cells without treatment or after 24 or 48 h of treatment with 20 μM UO126. Data are mean ± SD of 3 independent experiments.