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. 2010 Aug 12;53(15):5639-55.
doi: 10.1021/jm100383b.

Novel hinge binder improves activity and pharmacokinetic properties of BRAF inhibitors

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Novel hinge binder improves activity and pharmacokinetic properties of BRAF inhibitors

Alfonso Zambon et al. J Med Chem. .

Abstract

Mutated BRAF serine/threonine kinase is implicated in several types of cancer, with particularly high frequency in melanoma and colorectal carcinoma. We recently reported on the development of BRAF inhibitors based on a tripartite A-B-C system featuring an imidazo[4,5]pyridin-2-one group hinge binder. Here we present the design, synthesis, and optimization of a new series of inhibitors with a different A-B-C system that has been modified by the introduction of a range of novel hinge binders (A ring). The optimization of the hinge binding moiety has enabled the development of compounds with low nanomolar potencies in both BRAF inhibition and cellular assays. These compounds display optimal pharmacokinetic properties that warrant further in vivo investigations.

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