Biological and docking studies of topoisomerase IV inhibition by thiosemicarbazides

被引:0
|
作者
Agata Siwek
Paweł Stączek
Monika Wujec
Joanna Stefańska
Urszula Kosikowska
Anna Malm
Stefan Jankowski
Piotr Paneth
机构
[1] Medical University,Department of Organic Chemistry, Faculty of Pharmacy
[2] University of Lodz,Department of Genetics of Microorganisms
[3] Medical University,Department of Pharmaceutical Microbiology
[4] Medical University,Department of Pharmaceutical Microbiology, Faculty of Pharmacy
[5] Technical University of Lodz,Institute of Organic Chemistry
[6] Technical University of Lodz,Institute of Applied Radiation Chemistry
来源
Journal of Molecular Modeling | 2011年 / 17卷
关键词
Thiosemicarbazide derivative; Antibacterial activity; Bacterial topoisomerase IV; Enzyme inhibitor; Docking;
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中图分类号
学科分类号
摘要
4-Benzoyl-1-(4-methyl-imidazol-5-yl)-carbonylthiosemicarbazide (1) was synthesized, and its antibacterial and type IIA topoisomerase (DNA gyrase and topoisomerase IV) activity evaluated. (1) was found to have high therapeutic potential against opportunistic Gram-positive bacteria, and inhibitory activity against topoisomerase IV (IC50 = 90 μM) but not against DNA gyrase. An increase in activity against topoisomerase IV (IC50 = 14 μM) was observed when the imidazole moiety of (1) was replaced with the indole group in 4-benzoyl-1-(indol-2-yl)-carbonylthiosemicarbazide (2). However, (2) showed only weak antibacterial activity. Although the results of the bacterial type IIA topoisomerases inhibition study did not parallel antibacterial activities, our observations strongly imply that a 4-benzoylthiosemicarbazide scaffold can be developed into an efficient Gram-positive antibacterial targeting topoisomerase IV. The difference in activity against type IIA topoisomerases between (1) and (2) was further investigated by docking studies, which suggested that these compounds target the ATP binding pocket.
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页码:2297 / 2303
页数:6
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