Please use this identifier to cite or link to this item: https://cris.library.msu.ac.zw//handle/11408/4905
Title: Novel inhibitors of Mycobacterium tuberculosis GuaB2 identified by a target based high-throughput phenotypic screen
Authors: Cox, Jonathan A G
Mugumbate, Grace
Peral, Laura Vela-Glez Del
Jankute, Monika
Abrahams, Katherine A
Jervis, Peter
Jackenkroll, Stefan
Perez, Arancha
Alemparte, Carlos
Esquivias, Jorge
Lelièvre, Joël
Ramon, Fernando
Barros, David
Ballell, Lluis
Besra, Gurdyal S
Keywords: Antibiotics
High-throughput screening
Phenotypic screening
Target validation
Issue Date: 2016
Publisher: Nature Research
Series/Report no.: Scientific reports;Vol. 6,No. 38986
Abstract: High-throughput phenotypic screens have re-emerged as screening tools in antibiotic discovery. The advent of such technologies has rapidly accelerated the identification of 'hit' compounds. A pre-requisite to medicinal chemistry optimisation programmes required to improve the drug-like properties of a 'hit' molecule is identification of its mode of action. Herein, we have combined phenotypic screening with a biased target-specific screen. The inosine monophosphate dehydrogenase (IMPDH) protein GuaB2 has been identified as a drugable target in Mycobacterium tuberculosis, however previously identified compounds lack the desired characteristics necessary for further development into lead-like molecules. This study has identified 7 new chemical series from a high-throughput resistance-based phenotypic screen using Mycobacterium bovis BCG over-expressing GuaB2. Hit compounds were identified in a single shot high-throughput screen, validated by dose response and subjected to further biochemical analysis. The compounds were also assessed using molecular docking experiments, providing a platform for their further optimisation using medicinal chemistry. This work demonstrates the versatility and potential of GuaB2 as an anti-tubercular drug target.
URI: https://www.nature.com/articles/srep38986
http://hdl.handle.net/11408/4905
ISSN: 2045-2322
Appears in Collections:Research Papers

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