Predictive modeling targets thymidylate synthase ThyX in Mycobacterium tuberculosis

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作者
Kamel Djaout
Vinayak Singh
Yap Boum
Victoria Katawera
Hubert F. Becker
Natassja G. Bush
Stephen J. Hearnshaw
Jennifer E. Pritchard
Pauline Bourbon
Peter B. Madrid
Anthony Maxwell
Valerie Mizrahi
Hannu Myllykallio
Sean Ekins
机构
[1] LOB,Institute of Infectious Diseases and Molecular Medicine and Division of Medical Microbiology
[2] Ecole polytechnique,Microbiology Department
[3] CNRS,Department of Biological Chemistry
[4] INSERM,undefined
[5] Université Paris-Saclay,undefined
[6] MRC/NHLS/UCT Molecular Mycobacteriology Research Unit & DST/NRF Centre of Excellence for Biomedical TB Research,undefined
[7] Faculty of Health Sciences,undefined
[8] University of Cape Town,undefined
[9] Epicentre Mbarara Research Centre,undefined
[10] Faculty of Medicine,undefined
[11] Mbarara University of Science and Technology,undefined
[12] Sorbonne Universités,undefined
[13] UPMC Univ Paris 06,undefined
[14] John Innes Centre,undefined
[15] SRI International,undefined
[16] 333 Ravenswood Avenue,undefined
[17] Collaborative Drug Discovery,undefined
[18] 1633 Bayshore Highway,undefined
[19] Collaborations in Chemistry,undefined
[20] Present address: Inspiralis Ltd.,undefined
[21] Norwich Bioincubator,undefined
[22] Norwich Research Park,undefined
[23] Colney Lane,undefined
[24] Norwich NR4 7UH,undefined
[25] UK.,undefined
[26] Present address: Birkbeck College,undefined
[27] Univ. London WC1E 7HX,undefined
[28] UK.,undefined
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There is an urgent need to identify new treatments for tuberculosis (TB), a major infectious disease caused by Mycobacterium tuberculosis (Mtb), which results in 1.5 million deaths each year. We have targeted two essential enzymes in this organism that are promising for antibacterial therapy and reported to be inhibited by naphthoquinones. ThyX is an essential thymidylate synthase that is mechanistically and structurally unrelated to the human enzyme. DNA gyrase is a DNA topoisomerase present in bacteria and plants but not animals. The current study set out to understand the structure-activity relationships of these targets in Mtb using a combination of cheminformatics and in vitro screening. Here, we report the identification of new Mtb ThyX inhibitors, 2-chloro-3-(4-methanesulfonylpiperazin-1-yl)-1,4-dihydronaphthalene-1,4-dione) and idebenone, which show modest whole-cell activity and appear to act, at least in part, by targeting ThyX in Mtb.
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