Overview of the Development of DprE1 Inhibitors for Combating the Menace of Tuberculosis

Chikhale, Rupesh; Barmade, Mahesh A.; Murumkar, Prashant R.; Yadav, Mange Ram

doi:10.1021/acs.jmedchem.8b00281

Cited by 110 publications

(89 citation statements)

References 144 publications

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“…To date, more than 15 chemical classes of compounds inhibiting DprE1 have been reported. These classes encompass both covalent and noncovalent inhibitors, and although the covalent ones are the most successful, several noncovalent inhibitors with significant antitubercular activity have actually been described [45,46].…”

Section: Why Dpre1 Is a Promiscuous Targetmentioning

confidence: 99%

“…Currently, at least 11 different scaffolds have been reported as effective DprE1 inhibitors, either covalent and noncovalent, showing different efficacy in vitro, ex vivo and in vivo [46]. It is noteworthy that the majority of these compounds have been identified through phenotypic screening, then subjected to optimization processes.…”

Section: Dpre1 Inhibitors Which Are the Current Status And Future Pementioning

confidence: 99%

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Promiscuous Targets for Antitubercular Drug Discovery: The Paradigm of DprE1 and MmpL3

et al. 2020

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The development and spread of Mycobacterium tuberculosis multi-drug resistant strains still represent a great global health threat, leading to an urgent need for novel anti-tuberculosis drugs. Indeed, in the last years, several efforts have been made in this direction, through a number of high-throughput screenings campaigns, which allowed for the identification of numerous hit compounds and novel targets. Interestingly, several independent screening assays identified the same proteins as the target of different compounds, and for this reason, they were named “promiscuous” targets. These proteins include DprE1, MmpL3, QcrB and Psk13, and are involved in the key pathway for M. tuberculosis survival, thus they should represent an Achilles’ heel which could be exploited for the development of novel effective drugs. Indeed, among the last molecules which entered clinical trials, four inhibit a promiscuous target. Within this review, the two most promising promiscuous targets, the oxidoreductase DprE1 involved in arabinogalactan synthesis and the mycolic acid transporter MmpL3 are discussed, along with the latest advancements in the development of novel inhibitors with anti-tubercular activity.

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Section: Why Dpre1 Is a Promiscuous Targetmentioning

confidence: 99%

Section: Dpre1 Inhibitors Which Are the Current Status And Future Pementioning

confidence: 99%

Promiscuous Targets for Antitubercular Drug Discovery: The Paradigm of DprE1 and MmpL3

et al. 2020

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“…In MTB, the cell wall consists of the polymers of mycolyl-arabinogalactanpeptidoglycan, covalently connected with peptidoglycan and trehalose dimycolate that protects from stress, antibiotics and the hots immune systems [7]. The flavoenzyme decaprenylphosphoryl-β-d-ribose as a cofactor [8][9][10]. Thus, the catalytic activity of DprE1 is one of the potential drug targets in the development of tuberculosis therapy [2,4,7].…”

Section: Introductionmentioning

confidence: 99%

“…To improve the pharmacological properties of the compounds, chemical scaffold piperazine was added to BTZ. Further, the lead optimization of PBTZ derivatives results in the discovery of more potent compounds which are currently in clinical trials [5,8,11]. In this view, several structurally distinct chemical scaffolds are in drug screening as DprE1 inhibitors.…”

Section: Introductionmentioning

confidence: 99%

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Virtual screening and free energy estimation for identifying Mycobacterium tuberculosis flavoenzyme DprE1 inhibitors

Kumar

Srivastava

Prakash

et al. 2021

Journal of Molecular Graphics and Modelling

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Pyrazole–coumarin and pyrazole–quinoline chalcones as potential antitubercular agents

Kumar

Krishna

Sriram

et al. 2020

Archiv der Pharmazie

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Pyrazole, coumarin, and quinoline are medicinally important moieties. In this study, two series of novel pyrazole–coumarin chalcones and pyrazole–quinoline chalcones were synthesized using multiple‐step reactions. All the synthesized compounds were well characterized using different spectroscopic techniques including 1H and 13C nuclear magnetic resonance, high‐resolution mass spectroscopy, and electrospray ionization–mass spectrometry. The compounds were evaluated for their antitubercular activity against the Mycobacterium tuberculosis H37Rv strain using the microplate Alamar Blue assay, and the minimal inhibitory concentrations (MIC) of the compounds were determined. Among the 32 tested compounds, compounds 3e, 3u, and 7h showed an MIC value of 3.125 µg/ml, and they were found to be nontoxic. Molecular docking studies of the compounds with the enzyme DprE1 revealed the probable mechanism of action. The chalcone derivatives exhibited binding affinity values between −7.047 and −9.353 kcal/mol. ADME parameters were predicted using the QikProp module of the Schrödinger software, and these compounds exhibited good pharmacological and oral absorption properties.

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Overview of the Development of DprE1 Inhibitors for Combating the Menace of Tuberculosis

Cited by 110 publications

References 144 publications

Promiscuous Targets for Antitubercular Drug Discovery: The Paradigm of DprE1 and MmpL3

Promiscuous Targets for Antitubercular Drug Discovery: The Paradigm of DprE1 and MmpL3

Virtual screening and free energy estimation for identifying Mycobacterium tuberculosis flavoenzyme DprE1 inhibitors

Pyrazole–coumarin and pyrazole–quinoline chalcones as potential antitubercular agents

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