Pharmacophore-based molecular docking to account for ligand flexibility

Diane Joseph-McCarthy; Bert E Thomas 4th; Michael Belmarsh; Demetri Moustakas; Juan C Alvarez

doi:10.1002/prot.10266

Pharmacophore-based molecular docking to account for ligand flexibility

Proteins. 2003 May 1;51(2):172-88. doi: 10.1002/prot.10266.

Authors

Diane Joseph-McCarthy¹, Bert E Thomas 4th, Michael Belmarsh, Demetri Moustakas, Juan C Alvarez

Affiliation

¹ Wyeth Research, Biological Chemistry Department, Cambridge, Massachusetts 02140, USA. djoseph@wyeth.com

PMID: 12660987
DOI: 10.1002/prot.10266

Abstract

Rapid computational mining of large 3D molecular databases is central to generating new drug leads. Accurate virtual screening of large 3D molecular databases requires consideration of the conformational flexibility of the ligand molecules. Ligand flexibility can be included without prohibitively increasing the search time by docking ensembles of precomputed conformers from a conformationally expanded database. A pharmacophore-based docking method whereby conformers of the same or different molecules are overlaid by their largest 3D pharmacophore and simultaneously docked by partial matches to that pharmacophore is presented. The method is implemented in DOCK 4.0.

MeSH terms

Algorithms*
Binding Sites
Binding, Competitive
Databases, Protein
Drug Design*
HIV Protease / chemistry
Ligands
Methotrexate / chemistry
Methylurea Compounds / chemistry
Models, Molecular
NADP / chemistry
Protein Conformation
Proteins / chemistry
Pyridines / chemistry
Tetrahydrofolate Dehydrogenase / chemistry

Substances

A 79285
Ligands
Methylurea Compounds
Proteins
Pyridines
NADP
Tetrahydrofolate Dehydrogenase
HIV Protease
Methotrexate