Virtual medicinal chemistry: In silico pre-docking functional group transformation for discovery of novel inhibitors of botulinum toxin serotype A light chain

Article ID	Journal	Published Year	Pages	File Type
10591893	Bioorganic & Medicinal Chemistry Letters	2013	7 Pages	PDF

Abstract

A novel method for applying high-throughput docking to challenging metalloenzyme targets is described. The method utilizes information-based virtual transformation of library carboxylates to hydroxamic acids prior to docking, followed by compound acquisition, one-pot (two steps) chemical synthesis and in vitro screening. In two experiments targeting the botulinum neurotoxin serotype A metalloprotease light chain, hit rates of 32% and 18% were observed.

Keywords

Hydroxamic acid Biodefense Inhibitor design Drug design Virtual screening Metalloproteinase Botulinum neurotoxin

Related Topics

Physical Sciences and Engineering Chemistry Organic Chemistry

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Virtual medicinal chemistry: In silico pre-docking functional group transformation for discovery of novel inhibitors of botulinum toxin serotype A light chain

Authors

Sean O'Malley, Sina Sareth, Guan-Sheng Jiao, Seongjin Kim, April Thai, Lynne Cregar-Hernandez, Linda McKasson, Stephen A. Margosiak, Alan T. Johnson,