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DOI: 10.1016/j.ccr.2009.08.018
¤ OpenAccess: Hybrid
This work has “Hybrid” OA status. This means it is free under an open license in a toll-access journal.

Proteomic and Genetic Approaches Identify Syk as an AML Target

Cynthia K. Hahn,Jacob E. Berchuck,Kenneth N. Ross,Rose M. Kakoza,Karl R. Clauser,Anna C. Schinzel,Linda S. Ross,Ilene Galinsky,Tina Davis,Serena J. Silver,David E. Root,Richard Stone,Daniel J. DeAngelo,Martin Carroll,William C. Hahn,Steven A. Carr,Todd R. Golub,Andrew L. Kung,Kimberly Stegmaier

Syk
Myeloid leukemia
Phenotypic screening
2009
Cell-based screening can facilitate the rapid identification of compounds inducing complex cellular phenotypes. Advancing a compound toward the clinic, however, generally requires the identification of precise mechanisms of action. We previously found that epidermal growth factor receptor (EGFR) inhibitors induce acute myeloid leukemia (AML) differentiation via a non-EGFR mechanism. In this report, we integrated proteomic and RNAi-based strategies to identify their off-target, anti-AML mechanism. These orthogonal approaches identified Syk as a target in AML. Genetic and pharmacological inactivation of Syk with a drug in clinical trial for other indications promoted differentiation of AML cells and attenuated leukemia growth in vivo. These results demonstrate the power of integrating diverse chemical, proteomic, and genomic screening approaches to identify therapeutic strategies for cancer.
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    Proteomic and Genetic Approaches Identify Syk as an AML Target” is a paper by Cynthia K. Hahn Jacob E. Berchuck Kenneth N. Ross Rose M. Kakoza Karl R. Clauser Anna C. Schinzel Linda S. Ross Ilene Galinsky Tina Davis Serena J. Silver David E. Root Richard Stone Daniel J. DeAngelo Martin Carroll William C. Hahn Steven A. Carr Todd R. Golub Andrew L. Kung Kimberly Stegmaier published in 2009. It has an Open Access status of “hybrid”. You can read and download a PDF Full Text of this paper here.