Lead identification for modulators of multidrug resistance based on in silico screening with a pharmacophoric feature model

Author(s)
Thierry Langer, Monika Eder, Remy D. Hoffmann, Peter Chiba, Gerhard Ecker
Abstract

Considerable effort has been devoted to the characterization of P-glycoprotein - drug interaction in the past. Systematic quantitative structure-activity relationship (QSAR) studies identified both predictive physicochemical parameters and pharmacophoric substructures within homologous series of compounds. Comparative molecular field analysis (CoMFA) led to distinct 3D-QSAR models for propafenone and phenothiazine analogs. Recently, several pharmacophore models have been generated for diverse sets of ligands. Starting from a training set of 15 propafenone-type MDR-modulators, we established a chemical function-based pharmacophore model. The pharmacophoric features identified by this model were (i) one hydrogen bond acceptor, (ii) one hydrophobic area, (iii) two aromatic hydrophobic areas, and (iv) one positive ionizable group. In silica screening of the Derwent World Drug Index using the model led to identification of 28 compounds. Substances retrieved by database screening are diverse in structure and include dihydropyridines, chloroquine analogs, phenothiazines, and terfenadine. On the basis of its general applicability, the presented 3D-QSAR model allows in silica screening of virtual compound libraries to identify new potential lead compounds.

Organisation(s)
External organisation(s)
Leopold-Franzens-Universität Innsbruck
Journal
Archiv der Pharmazie
Volume
337
Pages
317-327
No. of pages
11
ISSN
0365-6233
Publication date
2004
Peer reviewed
Yes
Austrian Fields of Science 2012
3012 Pharmacy, Pharmacology, Toxicology
Portal url
https://ucrisportal.univie.ac.at/en/publications/9aae6607-7a87-4309-8001-63f35300025b