Structure Guided Lead Generation for M. tuberculosis Thymidylate Kinase (Mtb TMK): Discovery of 3-Cyanopyridone and 1,6-Naphthyridin-2-one as Potent Inhibitors

International audienceWe report the design and synthesis of a series of non-nucleoside MtbTMPK inhibitors (1-14) based on the gram-positive bacterial TMPK inhibitor hit compound 1. A practical synthesis was developed to access these analogues. Several compounds show promising MtbTMPK inhibitory potency and allow the establishment of a structure-activity relationship, which is helpful for further optimization

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“…s.,1H,4H,Ph),1H,Ph),4H,Ph) 7.69 (s,1H,11.18 (s,1H,NH). 13 5-methyl-1-(1-(3-phenoxybenzyl)piperidin-3-yl)pyrimidine-2,4(1H,3H)…”

Section: (R)-5-methyl-1-(1-(4-phenoxybenzyl)piperidin-3-yl)pyrimidinementioning

confidence: 99%

Elaboration of a proprietary thymidylate kinase inhibitor motif towards anti-tuberculosis agents

Song

Risseeuw

Froeyen

et al. 2016

Bioorganic & Medicinal Chemistry

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“…[18][19][20][21] Two novel classes, 3cyanopyridones and 1.6-naphthyridin-2-ones, were recently identified as MTB-TMK inhibitors via high-throughput screening and structural optimization to improve potency ( Figure 1). 22 These two scaffolds share a common substructure with thymidine, namely, the unsubstituted lactam functional group, which is important for the formation of hydrogen bonds with thymidylate kinase receptors.…”

Section: Introductionmentioning

confidence: 99%

In silico Design and Synthesis of Tetrahydropyrimidinones and Tetrahydropyrimidinethiones as Potential Thymidylate Kinase Inhibitors Exerting Anti-TB Activity Against Mycobacterium tuberculosis

Venugopala¹,

Tratrat²,

Pillay³

et al. 2020

DDDT

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Background and Purpose: Tuberculosis has been reported to be the worldwide leading cause of death resulting from a sole infectious agent. The emergence of multidrug-resistant tuberculosis and extensively drug-resistant tuberculosis has made the battle against the infection more difficult since most currently available therapeutic options are ineffective against these resistant strains. Therefore, novel molecules need to be developed to effectively treat tuberculosis disease. Preliminary docking studies revealed that tetrahydropyrimidinone derivatives have favorable interactions with the thymidylate kinase receptor. In the present investigation, we report the synthesis and the mycobacterial activity of several pyrimidinones and pyrimidinethiones as potential thymidylate kinase inhibitors. Methods: The title compounds (1a-d) and (2a-b) were synthesized by a one-pot three-component Biginelli reaction. They were subsequently characterized and used for whole-cell anti-TB screening against H37Rv and multidrug-resistant (MDR) strains of Mycobacterium tuberculosis (MTB) by the resazurin microplate assay (REMA) plate method. Molecular modeling was conducted using the Accelry's Discovery Studio 4.0 client program to explain the observed bioactivity of the compounds. The pharmacokinetic properties of the synthesized compounds were predicted and analyzed. Results: Of the compounds tested for anti-TB activity, pyrimidinone 1a and pyrimidinethione 2a displayed moderate activity against susceptible MTB H37Rv strains at 16 and 32 µg/mL, respectively. Only compound 2a was observed to exert modest activity at 128 µg/mL against MTB strains with cross-resistance to rifampicin and isoniazid. The presence of the trifluoromethyl group was essential to retain the inhibitory activity of compounds 1a and 2a. Molecular modeling studies of these compounds against thymidylate kinase targets demonstrated a positive correlation between the bioactivity and structure of the compounds. The in-silico ADME (absorption, distribution, metabolism, and excretion) prediction indicated favorable pharmacokinetic and drug-like properties for most compounds. Conclusion: Pyrimidinone 1a and pyrimidinethione 2a were identified as the leading compounds and can serve as a starting point to develop novel anti-TB therapeutic agents.

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“…However, phenotypic screens have not produced a substantial number of hits [2]. Fragment-based approaches have been able to produce potent lead compounds in vitro, some of which show good antimycobacterial activity despite the small number of dedicated studies in TB drug discovery using this methodology [48,49,54]. The fragments provide good starting points for rational compound elaboration that explores the protein hotspots.…”

Section: Discussionmentioning

confidence: 99%

“…Target-focused drug discovery campaigns performed on this enzyme have identified some inhibitors but all of the compounds obtained were either thymidine monophosphate analogs or contained a thymidine moiety [53]. Naik and colleagues performed a fragment screen using NMR and a biochemical assay that led to identification of new scaffolds inhibiting TMK [54]. They prioritized a 3-cyanopyridone-containing fragment for chemical elaboration (Figure 4a,b).…”

Section: Thymidylate Kinasementioning

confidence: 99%

“…The subsequent development of the fragment, supported by X-ray crystal structures of key compounds, allowed them to obtain nanomolar-potency lead compounds against this enzyme that retained high LE. These compounds differed from the substrate analogs and some proved to be active against M. tuberculosis [54] (Figure 4c-f). tuberculosis [57], with known high-affinity binders that show potent activity in vitro and in cell-based assays [58,59].…”

Section: Thymidylate Kinasementioning

confidence: 99%

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Targeting tuberculosis using structure-guided fragment-based drug design

Mendes

Blundell

2017

Drug Discovery Today

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Fragment-based drug discovery is now widely used in academia and industry to obtain small molecule inhibitors for a given target and is established for many fields of research including antimicrobials and oncology. Many molecules derived from fragment-based approaches are already in clinical trials and two - vemurafenib and venetoclax - are on the market, but the approach has been used sparsely in the tuberculosis field. Here, we describe the progress of our group and others, and examine the most recent successes and challenges in developing compounds with antimycobacterial activity.

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Structure Guided Lead Generation for M. tuberculosis Thymidylate Kinase (Mtb TMK): Discovery of 3-Cyanopyridone and 1,6-Naphthyridin-2-one as Potent Inhibitors

Cited by 39 publications

References 32 publications

Elaboration of a proprietary thymidylate kinase inhibitor motif towards anti-tuberculosis agents

Elaboration of a proprietary thymidylate kinase inhibitor motif towards anti-tuberculosis agents

<p>In silico Design and Synthesis of Tetrahydropyrimidinones and Tetrahydropyrimidinethiones as Potential Thymidylate Kinase Inhibitors Exerting Anti-TB Activity Against <em>Mycobacterium tuberculosis</em></p>

Targeting tuberculosis using structure-guided fragment-based drug design

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