2015
DOI: 10.1016/j.bmc.2015.11.017
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Discovery of benzothiazoles as antimycobacterial agents: Synthesis, structure–activity relationships and binding studies with Mycobacterium tuberculosis decaprenylphosphoryl-β-d-ribose 2′-oxidase

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Cited by 52 publications
(50 citation statements)
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“…In this context, DprE1 was found to have a very broad specificity for the electron acceptor, being able to use several compounds belonging to very different chemical classes. Indeed, the enzyme can reduce not only quinones, but also indophenols such as 2,6-dichlorophenolindophenol, or the phenoxazine moiety of resazurin, both compounds used in DprE1 activity assays [41,42], as well as different nitroaromatic moieties that characterize several covalent inhibitors of this enzyme [30,32,33,43,44].…”
Section: Why Dpre1 Is a Promiscuous Targetmentioning
confidence: 99%
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“…In this context, DprE1 was found to have a very broad specificity for the electron acceptor, being able to use several compounds belonging to very different chemical classes. Indeed, the enzyme can reduce not only quinones, but also indophenols such as 2,6-dichlorophenolindophenol, or the phenoxazine moiety of resazurin, both compounds used in DprE1 activity assays [41,42], as well as different nitroaromatic moieties that characterize several covalent inhibitors of this enzyme [30,32,33,43,44].…”
Section: Why Dpre1 Is a Promiscuous Targetmentioning
confidence: 99%
“…In this way, since the electron acceptor site is occupied, the enzyme is unable to reoxidize the flavin cofactor, resulting in being irreversibly inhibited [41,48] (Figure 1). phenoxazine moiety of resazurin, both compounds used in DprE1 activity assays [41,42], as well as different nitroaromatic moieties that characterize several covalent inhibitors of this enzyme [30,32,33,43,44]. To date, more than 15 chemical classes of compounds inhibiting DprE1 have been reported.…”
Section: Why Dpre1 Is a Promiscuous Targetmentioning
confidence: 99%
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“…DprE1 was characterized as the target of compound ( 34 ). In addition, this compound demonstrated safety profile with low cytotoxicity against human A549 cell line (IC 50 > 100 μM), negative Ames assay and moderate CYP isoform inhibition [60]. …”
Section: Antituberculosis Compoundsmentioning
confidence: 99%