Bisubstrate Adenylation Inhibitors of Biotin Protein Ligase from Mycobacterium tuberculosis

Duckworth, Benjamin P.; Geders, Todd W.; Tiwari, Divya; Boshoff, Helena I.; Sibbald, Paul A.; Barry, Clifton E.; Schnappinger, Dirk; Finzel, B.C.; Aldrich, Courtney C.

doi:10.1016/j.chembiol.2011.08.013

Cited by 84 publications

(146 citation statements)

References 52 publications

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“…This led to 5′-[N-(d-biotinoyl)sulfamoyl]amino-5′-deoxyadenosine (Bio-AMS), a BPL inhibitor with potent on-target whole-cell activity against drugsensitive and drug-resistant Mtb (17). Nevertheless, several important questions remained concerning its mechanism of action, mechanism of resistance in Mtb, pharmacokinetic (PK) properties, synergy with other antitubercular drugs, and, importantly, consequences of BPL inhibition in vivo.…”

Section: Introductionmentioning

confidence: 99%

“…We previously reported the design and characterization of potent inhibitors of biotin protein ligase (BPL), the enzyme responsible for covalently ligating biotin onto the ACCs (12)(13)(14)(15)(16)(17)(18)(19). This led to 5′-[N-(d-biotinoyl)sulfamoyl]amino-5′-deoxyadenosine (Bio-AMS), a BPL inhibitor with potent on-target whole-cell activity against drugsensitive and drug-resistant Mtb (17).…”

Section: Introductionmentioning

confidence: 99%

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Targeting protein biotinylation enhances tuberculosis chemotherapy

et al. 2018

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Targeting protein biotinylation enhances tuberculosis chemotherapy

et al. 2018

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“…As expected, the activity of BioAMS (but not of INH or ethambutol) against Mtb and M. smegmatis directly correlated with expression of BirA, and growth inhibition coincided with the depletion of biotinylated proteins. Together, these straightforward observations confirmed BirA as the primary target of BioAMS (Duckworth et al 2011). The second main advantage of target-based approaches is that they can survey a much larger chemical space than what can be covered in phenotypic screens, especially if fragment-based approaches are included (Scott et al 2012).…”

Section: Facilitating Target-based Drug Discoverymentioning

confidence: 63%

“…For example, a bisubstrate inhibitor (Bio-AMS) designed to inactivate the protein biotin ligase (BirA) was recently found to inhibit the growth of Mtb. The study conducted by Duckworth et al (2011) examined the impact of Bio-AMS on growth and biotinylation of proteins in M. smegmatis and Mtb. As expected, the activity of BioAMS (but not of INH or ethambutol) against Mtb and M. smegmatis directly correlated with expression of BirA, and growth inhibition coincided with the depletion of biotinylated proteins.…”

Section: Facilitating Target-based Drug Discoverymentioning

confidence: 99%

“…This was indeed observed for several conditional M. smegmatis knockdown mutants described recently. Underexpression of gyrase subunit A (GyrA, target of quinolones [Sugino et al 1977], Alr [Caceres et al 1997 (Duckworth et al 2011;Kim et al 2010;Wei et al 2011). Similar observations were made with Mtb, in which partial genetic inactivation of the biotin synthesis enzyme BioA or DHFR increased its susceptibility toward the novel inhibitors of these enzymes (Shi et al 2011;Kumar et al 2012).…”

Section: Linking Small Molecules To Candidate Targets By Increasing Omentioning

confidence: 99%

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Genetic Approaches to Facilitate Antibacterial Drug Development

Schnappinger

2015

Cold Spring Harb Perspect Med

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Design, synthesis, molecular docking, and biological evaluation of coumarin‐thymidine analogs as potent anti‐TB agents

Reddy

Sinha

Kurjogi

et al. 2023

Archiv der Pharmazie

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With the intent to discover new antituberculosis (TB) compounds, coumarinthymidine analogs were synthesized using second-order nucleophilic substitution reactions of bromomethyl coumarin with thymidine. The newly synthesized coumarin-thymidine conjugates (1a-l) were characterized using IR, NMR, GC-MS, and CHN elemental analysis. The novel conjugates were found to exhibit potent anti-TB activity against the Mycobacterium tuberculosis H 37 Rv strain, with minimum inhibitory concentrations (MIC) of the active compounds ranging between 0.012 and 0.482 µM. Compound 1k was established as the most active candidate with a MIC of 0.012 µM. The toxicity study on HEK cells confirmed the nontoxic nature of compounds 1e, 1h, 1i, 1j, and 1k. Also, the most active compounds (1k, 1j, and 1e) were stable in the pH range from 2.5 to 10, indicating compatibility with the biophysical environment. Based on the pK a studies, compounds 1k, 1j, and 1e are capable of crossing lipid-membrane barriers and acting on target cells. Molecular docking studies on the M. tuberculosis β-oxidation trifunctional enzyme (PDB ID: 7O4V) were conducted to investigate the mechanisms of anti-TB activity. All compounds showed excellent hydrogen binding interactions and exceptional docking scores against M. tuberculosis, which was in accordance with the results.Compounds 1a-l possessed excellent affinity to proteins, with binding energies ranging from −7.4 to −8.7 kcal/mol.

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Bisubstrate Adenylation Inhibitors of Biotin Protein Ligase from Mycobacterium tuberculosis

Cited by 84 publications

References 52 publications

Targeting protein biotinylation enhances tuberculosis chemotherapy

Targeting protein biotinylation enhances tuberculosis chemotherapy

Genetic Approaches to Facilitate Antibacterial Drug Development

Design, synthesis, molecular docking, and biological evaluation of coumarin‐thymidine analogs as potent anti‐TB agents

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