A Structural and Energetic Model for the Slow-Onset Inhibition of the <i>Mycobacterium tuberculosis</i> Enoyl-ACP Reductase InhA

Li, Huei Jiun; Lai, Cheng Tsung; Pan, Pan; Yu, Weixuan; Liu, Nina; Bommineni, Gopal R.; García‐Díaz, Miguel; Simmerling, Carlos; Tonge, Peter J.

doi:10.1021/cb400896g

Cited by 60 publications

(107 citation statements)

References 55 publications

Supporting

Mentioning

103

Contrasting

Order By: Relevance

“…6). Furthermore, the structure of InhA in complex with the 4-pyridone PT155 shares a very similar open SBL conformation with the substrate-bound form of this enzyme (74,76). As expected based on these considerations, the SAR and predicted binding mode for the 4-pyridones is highly reminiscent of the 2-pyridone series, but 4-pyridones possess superior potency at the enzymatic and cellular levels (Tables 1 and 2).…”

Section: Discussionmentioning

confidence: 57%

“…Similar to the ecFabI-NADH-CG400549 structure, the substrate-binding loop was found to be disordered or in a very open conformation in these ecFabI and bpFabI structures, respectively. Interestingly, an open SBL conformation was very recently also observed in the structure of PT155 bound to InhA (74).…”

Section: -Pyridone Pt166 Is a Potent Fabi Inhibitor With Extended Spmentioning

confidence: 63%

See 1 more Smart Citation

Rational Design of Broad Spectrum Antibacterial Activity Based on a Clinically Relevant Enoyl-Acyl Carrier Protein (ACP) Reductase Inhibitor

Schiebel

Chang

Shah

et al. 2014

Journal of Biological Chemistry

Self Cite

View full text Add to dashboard Cite

Background:The FabI inhibitor CG400549 is a promising new anti-staphylococcal drug candidate with recently validated human efficacy. Results: We revealed the molecular determinants conferring S. aureus FabI selectivity to rationally design a compound with an improved antibacterial activity spectrum. Conclusion:The 4-pyridone PT166 represents a critical step toward Gram-negative and mycobacterial coverage. Significance: We provide an approach to expand the spectrum of antimicrobial activity.

show abstract

Section: Discussionmentioning

confidence: 57%

Section: -Pyridone Pt166 Is a Potent Fabi Inhibitor With Extended Spmentioning

confidence: 63%

Rational Design of Broad Spectrum Antibacterial Activity Based on a Clinically Relevant Enoyl-Acyl Carrier Protein (ACP) Reductase Inhibitor

Schiebel

Chang

Shah

et al. 2014

Journal of Biological Chemistry

Self Cite

View full text Add to dashboard Cite

show abstract

“…In lieu of X-ray crystal structures, we offer the docking calculations provide an understanding of reasonable inhibitor binding modes to InhA, given the assumptions made by the software. Since InhA is a flexible enzyme which contains a substrate-binding loop that samples multiple distinct conformations when it forms a lid on the active site, [49] several conformations of InhA from multiple chains of four different ligand-bound crystal structures of InhA were utilized as targets for these docking studies. 2X23 [50] and 3FNH [32] are both bound to triclosan derivatives, while 4COD [37] and 4BQP [38] are new crystal structures of InhA bound to structurally distinct lead compounds from GlaxoSmithKline and AstraZeneca, respectively.…”

Section: Resultsmentioning

confidence: 99%

Biological Evaluation of Potent Triclosan‐Derived Inhibitors of the Enoyl–Acyl Carrier Protein Reductase InhA in Drug‐Sensitive and Drug‐Resistant Strains of Mycobacterium tuberculosis

Stec

Vilchèze

Lun³

et al. 2014

ChemMedChem

View full text Add to dashboard Cite

New triclosan (TRC) analogs were evaluated for their activity against the enoyl-acyl carrier protein reductase InhA in Mycobacterium tuberculosis (Mtb). TRC is a well-known inhibitor of InhA and specific modifications to its positions 5 and 4′ afforded twenty-seven derivatives; of these compounds seven derivatives showed an improved potency in comparison to TRC. These analogs were active against both drug-susceptible and drug-resistant Mtb strains. The most active compound in this series, 3, had an MIC value of 0.6 μg/mL (1.5 μM) against wild-type Mtb. At a concentration equal to its MIC, this molecule inhibited the purified InhA enzyme to the extent of 98%, and it showed an IC50 value of 90 nM. Compounds 3 and 14 were able to inhibit the biosynthesis of mycolic acids. Furthermore, mc24914, an Mtb strain overexpressing inhA, was resistant to the compounds 3 and 14, supporting the notion that InhA is the likely molecular target of the TRC derivatives presented herein.

show abstract

“…5 The figure shows a simple one-step mechanism, although in many cases slow-binding inhibitors operate through a two-step induced-fit mechanism. 13,15,28−31 …”

Section: The Thermodynamics and Kinetics Of Drug–target Interactionsmentioning

confidence: 99%

Drug–Target Kinetics in Drug Discovery

Tonge

2017

ACS Chem. Neurosci.

Self Cite

214

235

View full text Add to dashboard Cite

The development of therapies for the treatment of neurological cancer faces a number of major challenges including the synthesis of small molecule agents that can penetrate the blood brain barrier (BBB). Given the likelihood that in many cases drug exposure will be lower in the CNS than in systemic circulation, it follows that strategies should be employed that can sustain target engagement at low drug concentration. Time dependent target occupancy is a function of both the drug and target concentration as well as the thermodynamic and kinetic parameters that describe the binding reaction coordinate, and sustained target occupancy can be achieved through structural modifications that increase target (re)binding and/or that decrease the rate of drug dissociation. The discovery and deployment of compounds with optimized kinetic effects requires information on the structure-kinetic relationships that modulate the kinetics of binding, and the molecular factors that control the translation of drug-target kinetics to time-dependent drug activity in the disease state. This review first introduces the potential benefits of drug-target kinetics, such as the ability to delineate both thermodynamic and kinetic selectivity, and then describes factors, such as target vulnerability, that impact the utility of kinetic selectivity. The review concludes with a description of a mechanistic PK/PD model that integrates drug-target kinetics into predictions of drug activity.

show abstract

A Structural and Energetic Model for the Slow-Onset Inhibition of the Mycobacterium tuberculosis Enoyl-ACP Reductase InhA

Cited by 60 publications

References 55 publications

Rational Design of Broad Spectrum Antibacterial Activity Based on a Clinically Relevant Enoyl-Acyl Carrier Protein (ACP) Reductase Inhibitor

Rational Design of Broad Spectrum Antibacterial Activity Based on a Clinically Relevant Enoyl-Acyl Carrier Protein (ACP) Reductase Inhibitor

Biological Evaluation of Potent Triclosan‐Derived Inhibitors of the Enoyl–Acyl Carrier Protein Reductase InhA in Drug‐Sensitive and Drug‐Resistant Strains of Mycobacterium tuberculosis

Drug–Target Kinetics in Drug Discovery

Contact Info

Product

Resources

About