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Novel Antitubercular 6-Dialkylaminopyrimidine Carboxamides from Phenotypic Whole-Cell High Throughput Screening of a SoftFocus Library: Structure-Activity Relationship and Target Identification Studies.


ABSTRACT: A BioFocus DPI SoftFocus library of ?35?000 compounds was screened against Mycobacterium tuberculosis (Mtb) in order to identify novel hits with antitubercular activity. The hits were evaluated in biology triage assays to exclude compounds suggested to function via frequently encountered promiscuous mechanisms of action including inhibition of the QcrB subunit of the cytochrome bc1 complex, disruption of cell-wall homeostasis, and DNA damage. Among the hits that passed this screening cascade, a 6-dialkylaminopyrimidine carboxamide series was prioritized for hit to lead optimization. Compounds from this series were active against clinical Mtb strains, while no cross-resistance to conventional antituberculosis drugs was observed. This suggested a novel mechanism of action, which was confirmed by chemoproteomic analysis leading to the identification of BCG_3193 and BCG_3827 as putative targets of the series with unknown function. Initial structure-activity relationship studies have resulted in compounds with moderate to potent antitubercular activity and improved physicochemical properties.

SUBMITTER: Wilson CR 

PROVIDER: S-EPMC5748279 | biostudies-literature | 2017 Dec

REPOSITORIES: biostudies-literature

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Novel Antitubercular 6-Dialkylaminopyrimidine Carboxamides from Phenotypic Whole-Cell High Throughput Screening of a SoftFocus Library: Structure-Activity Relationship and Target Identification Studies.

Wilson Colin R CR   Gessner Richard K RK   Moosa Atica A   Seldon Ronnett R   Warner Digby F DF   Mizrahi Valerie V   Soares de Melo Candice C   Simelane Sandile B SB   Nchinda Aloysius A   Abay Efrem E   Taylor Dale D   Njoroge Mathew M   Brunschwig Christel C   Lawrence Nina N   Boshoff Helena I M HIM   Barry Clifton E CE   Sirgel Frederick A FA   van Helden Paul P   Harris C John CJ   Gordon Richard R   Ghidelli-Disse Sonja S   Pflaumer Hannah H   Boesche Markus M   Drewes Gerard G   Sanz Olalla O   Santos Gracia G   Rebollo-Lopez Maria José MJ   Urones Beatriz B   Selenski Carolyn C   Lafuente-Monasterio Maria Jose MJ   Axtman Matthew M   Lelièvre Joël J   Ballell Lluis L   Mueller Rudolf R   Street Leslie J LJ   Ghorpade Sandeep R SR   Chibale Kelly K  

Journal of medicinal chemistry 20171207 24


A BioFocus DPI SoftFocus library of ∼35 000 compounds was screened against Mycobacterium tuberculosis (Mtb) in order to identify novel hits with antitubercular activity. The hits were evaluated in biology triage assays to exclude compounds suggested to function via frequently encountered promiscuous mechanisms of action including inhibition of the QcrB subunit of the cytochrome bc<sub>1</sub> complex, disruption of cell-wall homeostasis, and DNA damage. Among the hits that passed this screening  ...[more]

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