Directed Discovery of Agents Targeting the Met Tyrosine Kinase Domain by Virtual Screening

Author:

Peach, M. L.

Tan, N.

Choyke, S. J.

Giubellino, A.

Athauda, G.

Burke, T. R.

Nicklaus, M. C.

Bottaro, D. P.
Author Address

Tan, Nelly, Choyke, Sarah J.; Giubellino, Alessio, Athauda, Gagani, Bottaro, Donald P.] NCI, Urol Oncol Branch, Ctr Canc Res, Bethesda, MD 20892 USA. [Peach, Megan L.] SAIC Frederick Inc, Basic Res Program, NCI Frederick, Frederick, MD 21702 USA. [Burke, Terrence R., Jr.; Nicklaus, Marc C.] NCI, Med Chem Lab, Ctr Canc Res, Ft Detrick, MD 21702 USA.

Abstract:

Hepatocyte growth factor (HGF) is an important regulator of normal development and homeostasis, and dysregulated signaling through the HGF receptor, Met, contributes to tumorigenesis, tumor progression, and metastasis in numerous human malignancies. The development of selective small-molecule inhibitors of oncogenic tyrosine Kinases (TK) has led to well-tolerated, targeted therapies for a growing number of cancer types. To identify selective Met TK inhibitors, we used a high-throughput virtual screen of the 13.5 million compound ChemNavigator database to find compounds most likely to bind to the Met ATP binding site and to form several critical interactions with binding site residues predicted to stabilize the kinase domain in its inactive conformation. Subsequent biological screening of 70 in silico hit structures using cell-free and intact cell assays identified three active compounds with micromolar IC50 values. The predicted binding modes and target selectivity of these compounds are discussed and compared to other known Met TK inhibitors.

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