Abstract
Glycosyltransferase is an essential and easily accessible drug target for antibiotic-resistance. The crystal structures of glycosyltransferase (GT51) provide us with the chance to develop new antibiotics that interrupt a yet unexplored molecular target. Based on the crystal structure of GT51, we have carried out computational screening of GT51 in order to look for novel GT51 inhibitors. The present study was accomplished by using advance docking and scoring methodology. It is the first example of virtual screening of GT51 inhibitors. Two docking procedures (Surflex-Dock and FlexX-Pharm dockings) were applied and nine novel potential leads are proposed after thorough examination by a combination of methods.