| Literature DB >> 30962087 |
Reema K Thalji1, Kaushik Raha1, Daniele Andreotti2, Anna Checchia2, Haifeng Cui1, Giovanni Meneghelli2, Roberto Profeta2, Federica Tonelli2, Simona Tommasi2, Tania Bakshi1, Brian T Donovan1, Alison Howells3, Shruti Jain3, Christopher Nixon1, Geoffrey Quinque1, Lynn McCloskey1, Benjamin D Bax4, Margarete Neu4, Pan F Chan1, Robert A Stavenger5.
Abstract
A series of DNA gyrase inhibitors were designed based on the X-ray structure of a parent thiophene scaffold with the objective to improve biochemical and whole-cell antibacterial activity, while reducing cardiac ion channel activity. The binding mode and overall design hypothesis of one series was confirmed with a co-crystal structure with DNA gyrase. Although some analogs retained both biochemical activity and whole-cell antibacterial activity, we were unable to significantly improve the activity of the series and analogs retained activity against the cardiac ion channels, therefore we stopped optimization efforts.Entities:
Keywords: Antibacterial; Topoisomerase
Year: 2019 PMID: 30962087 DOI: 10.1016/j.bmcl.2019.03.029
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823