Disruption of Angiogenesis and Tumor Growth with an Orally Active Drug That Stabilizes the Inactive State of PDGFRbeta/B-RAF

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2010 Feb 16

PMID 20154271

Citations 25

Authors

Eric A Murphy

David J Shields

Konstantin Stoletov

Elena Dneprovskaia

Michele McElroy

Joshua I Greenberg

Jeff Lindquist

Lisette M Acevedo

Sudarshan Anand

Bharat Kumar Majeti

Igor Tsigelny

Adrian Saldanha

Breda Walsh

Robert M Hoffman

Michael Bouvet

Richard L Klemke

Peter K Vogt

Lee Arnold

Wolfgang Wrasidlo

David A Cheresh

Affiliations

Soon will be listed here.

Abstract

Kinases are known to regulate fundamental processes in cancer including tumor proliferation, metastasis, neovascularization, and chemoresistance. Accordingly, kinase inhibitors have been a major focus of drug development, and several kinase inhibitors are now approved for various cancer indications. Typically, kinase inhibitors are selected via high-throughput screening using catalytic kinase domains at low ATP concentration, and this process often yields ATP mimetics that lack specificity and/or function poorly in cells where ATP levels are high. Molecules targeting the allosteric site in the inactive kinase conformation (type II inhibitors) provide an alternative for developing selective inhibitors that are physiologically active. By applying a rational design approach using a constrained amino-triazole scaffold predicted to stabilize kinases in the inactive state, we generated a series of selective type II inhibitors of PDGFRbeta and B-RAF, important targets for pericyte recruitment and endothelial cell survival, respectively. These molecules were designed in silico and screened for antivascular activity in both cell-based models and a Tg(fli1-EGFP) zebrafish embryogenesis model. Dual inhibition of PDGFRbeta and B-RAF cellular signaling demonstrated synergistic antiangiogenic activity in both zebrafish and murine models of angiogenesis, and a combination of previously characterized PDGFRbeta and RAF inhibitors validated the synergy. Our lead compound was selected as an orally active molecule with favorable pharmacokinetic properties which demonstrated target inhibition in vivo leading to suppression of murine orthotopic tumors in both the kidney and pancreas.

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