Author:
Kumar Anuradha,Chettiar Somsundaram,Brown Brian S.,Early Julie,Ollinger Juliane,Files Megan,Bailey Mai A.,Korkegian Aaron,Dennison Devon,McNeil Matthew,Metz James,Osuma Augustine,Curtin Michael,Kunzer Aaron,Freiberg Gail,Bruncko Milan,Kempf Dale,Parish Tanya
Abstract
AbstractWe performed a high-throughput phenotypic whole cell screen of Mycobacterium tuberculosis against a diverse chemical library of approximately 100,000 compounds from the AbbVie corporate collection and identified 24 chemotypes with anti-tubercular activity. We selected two series for further exploration and conducted structure–activity relationship studies with new analogs for the 4-phenyl piperidines (4PP) and phenylcyclobutane carboxamides (PCB). Strains with mutations in MmpL3 demonstrated resistance to both compound series. We isolated resistant mutants for the two series and found mutations in MmpL3. These data suggest that MmpL3 is the target, or mechanism of resistance for both series.
Funder
Bill and Melinda Gates Foundation
Publisher
Springer Science and Business Media LLC
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