A combined 3D QSAR and pharmacophore-based virtual screening for the identification of potent p38 MAP kinase inhibitors: an in silico approach

Abstract

p38 kinase plays a vital role in inflammation mediated by tumor necrosis factor-α and interleukin-1β pathways. Inhibition of p38 kinase provides an effective way to treat inflammatory diseases. 3D-QSAR study was performed to obtain reliable comparative molecular field analysis (CoMFA) and comparative molecular similarity indices analysis (CoMSIA) models for a series of p38 inhibitors with three different alignment methods (Receptor based, atom by atom matching, and pharmacophore based). Among the different alignment methods, better statistics were obtained with receptor-based alignment (CoMFA: q 2 = 0.777, r 2 = 0.958; CoMSIA: q 2 = 0.782, r 2 = 0.927). Superposing CoMFA/CoMSIA contour maps on the p38 active site gave a valuable insight to understand physical factors which are important for binding. In addition, this pharmacophore model was used as a 3D query for virtual screening against NCI database. The hit compounds were further filtered by docking and scoring, and their biological activities were predicted by CoMFA and CoMSIA models.