Structure-based drug design enables conversion of a DFG-in binding CSF-1R kinase inhibitor to a DFG-out binding mode.

Marvin Jay Meyers,Matthew James Pelc,Satwik Kamtekar,Jacqueline E. Day,Gennadiy I. Poda,Molly K. Hall,Marshall L. Michener,Beverly A. Reitz,Karl J. Mathis,Betsy S. Pierce,Mihir D. Parikh,Deborah A. Mischke,Scott A. Long,John J. Parlow,David R. Anderson,Atli Thorarensen

Structure-based drug design enables conversion of a DFG-in binding CSF-1R kinase inhibitor to a DFG-out binding mode.

2010

Marvin Jay Meyers
Matthew James Pelc
Satwik Kamtekar
Jacqueline E. Day
Gennadiy I. Poda
Molly K. Hall
Marshall L. Michener
Beverly A. Reitz
Karl J. Mathis
Betsy S. Pierce
Mihir D. Parikh
Deborah A. Mischke
Scott A. Long
John J. Parlow
David R. Anderson
Atli Thorarensen

The work described herein demonstrates the utility of structure-based drug design (SBDD) in shifting the binding mode of an HTS hit from a DFG-in to a DFG-out binding mode resulting in a class of novel potent CSF-1R kinase inhibitors suitable for lead development.

Keywords:

Drug
Combinatorial chemistry
Plasma protein binding
Kinase
Binding site
Hydrogen bond
Biochemistry
Chemistry
High-Throughput Screening Assays
Transferase
Phosphotransferases
structure based
molecular conformation

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