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The SFKs confer BRAF inhibitor resistance in BRAF-mutant melanoma cells. The SFKs confer BRAF inhibitor resistance in BRAF-mutant melanoma cells. A, phospho-protein.

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Presentation on theme: "The SFKs confer BRAF inhibitor resistance in BRAF-mutant melanoma cells. The SFKs confer BRAF inhibitor resistance in BRAF-mutant melanoma cells. A, phospho-protein."— Presentation transcript:

1 The SFKs confer BRAF inhibitor resistance in BRAF-mutant melanoma cells.
The SFKs confer BRAF inhibitor resistance in BRAF-mutant melanoma cells. A, phospho-protein array from A375 and A375/R cells. B, quantitation of phospho-array data for LYN, FYN, YES, and FAK from A. C, Western blot analysis showing LYN phosphorylation (pLYN) in A375(X), A375(X)/R, A375, A375/R, Colo829, and Colo829/R cells. Tubulin, loading control. D, proliferation of A375, A375/R, A375(X), A375(X)/R, Colo829, and Colo829/R cells in the presence of dasatinib and saracatinib. Values are relative to DMSO, and IC50 values are presented as mean (μmol/L; n = 3) ± SEM (34). E, graph showing growth of A375(X)/R xenografts in nude mice treated with vehicle, PLX4720 (25 mg/kg/d orally), or dasatinib (75 mg/kg/d orally). Drug treatments commenced when tumors were 40 to 50 mm3 and mean tumor volumes ± SEM (34) are shown (n = 6 mice/group). F, Western blot analyses for phospho-SFK Y416 (pSFK) and SRC in A375/R, A375(X)/R, and Colo829/R cells treated with DMSO or dasatinib (DAS; 20 nmol/L, 24 hours). G, photomicrographs showing pSFK staining in A375(X)/R xenografts from mice after 30 days of treatment with vehicle or dasatinib (75 mg/kg/d orally). Scale bar, 50 μm. Maria R. Girotti et al. Cancer Discovery 2013;3: ©2013 by American Association for Cancer Research


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