Discovery of a Novel Antimicrobial Agent by the Virtual Screening of a Library of Small Molecules.

A virtual screening approach based upon a combination of docking and pharmacophore methods was utilized on a library of 1.4 million molecules to identify novel antimicrobial agents, which may potentially act via inhibition of the caseinolytic protease. Using this method, compound 6 was found to be bactericidal against three staphylococcal species (minimum inhibitory concentration (MIC)=4-16 μg/mL).

Structure-Based Scaffold Repurposing toward the Discovery of Novel Cholinesterase Inhibitors.

Cholinesterases (ChE) are well-known drug targets for the treatment of Alzheimer's disease (AD). In continuation of work to develop novel cholinesterase inhibitors, we utilized a structure-based scaffold repurposing approach and discovered six novel ChE inhibitors from our recently developed DNA gyrase inhibitor library. Among the identified hits, two compounds (denoted and ) were found to be the most potent inhibitor of acetylcholinesterase (AChE, IC = 6.