Identification of Compounds with Nanomolar Binding Affinity for Checkpoint Kinase-1 Using Knowledge-based Virtual Screening

Overview

Journal J Med Chem

Publisher American Chemical Society

Specialty Chemistry

Date 2004 Apr 2

PMID 15055996

Citations 19

Authors

Paul D Lyne

Peter W Kenny

David A Cosgrove

Chun Deng

Sonya Zabludoff

John J Wendoloski

Susan Ashwell

Affiliations

Soon will be listed here.

Abstract

A virtual screen of a subsection of the AstraZeneca compound collection was performed for checkpoint kinase-1 (Chk-1 kinase) using a knowledge-based strategy. This involved initial filtering of the compound collection by application of generic physical properties followed by removal of compounds with undesirable chemical functionality. Subsequently, a 3-D pharmacophore screen for compounds with kinase binding motifs was applied. A database of approximately 200K compounds remained for docking into the active site of Chk-1 kinase, using the FlexX-Pharm program. For each compound that docked successfully into the binding site, up to 100 poses were saved. These poses were then postfiltered using a customized consensus scoring scheme for a kinase, followed by visual inspection of a selection of the docked compounds. This resulted in 103 compounds being ordered for testing in the project assay, and 36 of these (corresponding to four chemical classes) were found to inhibit the enzyme in a dose-response fashion with IC(50) values ranging from 110 nM to 68 microM.

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