Characterization of ATP-independent ERK Inhibitors Identified Through in Silico Analysis of the Active ERK2 Structure

Overview

Journal Bioorg Med Chem Lett

Specialty Biochemistry

Date 2006 Sep 27

PMID 17000106

Citations 30

Authors

Fengming Chen

Chad N Hancock

Alba T Macias

Joseph Joh

Kimberly Still

Shijun Zhong

Alexander D MacKerell Jr

Paul Shapiro

Affiliations

Soon will be listed here.

Abstract

The extracellular signal-regulated kinases (ERK1 and ERK2) are important mediators of cell proliferation. Constitutive activation of the ERK proteins plays a critical role in the proliferation of many human cancers. Taking advantage of recently identified substrate docking domains on ERK2, we have used computer-aided drug design (CADD) to identify novel low molecular weight compounds that interact with ERK2 in an ATP-independent manner and disrupt substrate-specific interactions. In the current study, a CADD screen of the 3D structure of active phosphorylated ERK2 protein was used to identify inhibitory compounds. We tested 13 compounds identified by the CADD screen in ERK-specific phosphorylation, cell proliferation, and binding assays. Of the 13 compounds tested, 4 compounds strongly inhibited ERK-mediated phosphorylation of ribosomal S6 kinase-1 (Rsk-1) and/or the transcription factor Elk-1 and inhibited the proliferation of HeLa cervical carcinoma cells with IC(50) values in the 2-10 microM range. These studies demonstrate that CADD can be used to identify lead compounds for development of novel non-ATP-dependent inhibitors selective for active ERK and its interactions with substrates involved in cancer cell proliferation.

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