Quantum Mechanics/Molecular Mechanics Studies on the Catalytic Mechanism of a Novel Esterase (FmtA) of <i>Staphylococcus aureus</i>

Dalal, Vikram; Golemi-Kotra, Dasantila; Kumar, Pravindra

doi:10.1021/acs.jcim.2c00057

Cited by 31 publications

(16 citation statements)

References 80 publications

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“…1.XX of the Avogadro molecular builder tool [ 43 ], and was subsequently converted to PDB format using the PyMOL Molecular Graphics System. The ligand (RXn-02) and receptors (target proteins) were prepared for the addition of hydrogen atoms (polar only), removal of water (H 2 0) molecules, and the addition of Kollman charges [ [44] , [45] , [46] ], prior to the docking simulation according to the methods described in previous studies [ 47 , 48 ]. Docking simulations were conducted using the default settings of AutoDock Vina (vers.…”

Section: Introductionmentioning

confidence: 99%

Identification of a novel immune-inflammatory signature of COVID-19 infections, and evaluation of pharmacokinetics and therapeutic potential of RXn-02, a novel small-molecule derivative of quinolone

Lawal

Kuo

Sumitra

et al. 2022

Computers in Biology and Medicine

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Section: Introductionmentioning

confidence: 99%

Identification of a novel immune-inflammatory signature of COVID-19 infections, and evaluation of pharmacokinetics and therapeutic potential of RXn-02, a novel small-molecule derivative of quinolone

Lawal

Kuo

Sumitra

et al. 2022

Computers in Biology and Medicine

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“…The conserved residues of the catalytic triad have different roles: Ser functions as a nucleophile, Lys works in acylation/deacylation, while Tyr holds the substrate in the course of hydrolysis of WTA . The QM/MM study suggested that the release of d -Alanine from WTA involves the formation of an acyl–enzyme complex and two tetrahedral intermediate complexes, which are stabilized via oxyanion hole residues (backbone amide of Ser127 and Gly344) . Therefore, in FmtA, the first motif residues (Ser127 and Lys130) were involved in catalysis and charge neutralization; second motif (Tyr211 and Asp213) in holding the substrate; and third motif (Asn343 and Gly344) is crucial for the stability and charge neutralization of WTA …”

Section: Discussionmentioning

confidence: 99%

“…DFT calculation was done to evaluate the polarity of drugs (gemifloxacin, paromomycin, streptomycin, and tobramycin) . The molecular electrostatic potential and molecular orbital energies were assessed by using B3LYP with the basis set of 6-311G (d,p), as done by Dalal et al ,,,, Furthermore, quantum mechanics/molecular mechanics (QM/MM) estimations for FmtA–drug(s) complexes were conducted using our own N-layered integrated molecular orbital and molecular mechanics (ONIOM) method, as done by Dalal et al ,,, The inhibitor and side chain atoms of Ser127, Lys130, Tyr211, and Asp213 were considered in the QM layer, whereas the remaining part of the protein was put in the MM layer. The enthalpy (Δ H ), relative Gibbs free energy (Δ G ), and entropy (Δ S ) were assessed by ONIOM (B3LYP/6-311G(d,p): AMBER).…”

Section: Methodsmentioning

confidence: 99%

“…The conserved motifs comprising Ser, Lys, and Tyr are crucial for the functioning of FmtA, that is, Ser is known to function as a nucleophile, Lys works in acylation/deacylation, while Tyr holds the substrate in the course of hydrolysis of WTA. Further, the quantum mechanics/molecular mechanics (QM/MM) study showed that the backbone amides of Ser127 and Gly344 act as oxyanion hole residues to stabilize the tetrahedral intermediates for the catalysis of WTA by FmtA …”

Section: Introductionmentioning

confidence: 99%

“…Further, the quantum mechanics/molecular mechanics (QM/ MM) study showed that the backbone amides of Ser127 and Gly344 act as oxyanion hole residues to stabilize the tetrahedral intermediates for the catalysis of WTA by FmtA. 24 In the current study, we have utilized the available crystal structure of FmtA (PDB ID: 5ZH8) for performing structurebased virtual screening against the drugs of e-LEA3D. The binding affinity of the screened compounds (gemifloxacin, paromomycin, streptomycin, and tobramycin) was crossconfirmed by molecular docking studies utilizing HADDOCK and AutoDockTools.…”

Section: Introductionmentioning

confidence: 99%

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Drug-Repurposing Approach To Combat Staphylococcus aureus: Biomolecular and Binding Interaction Study

et al. 2022

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Staphylococcus aureus is considered as one of the most widespread bacterial pathogens and continues to be a prevalent cause of mortality and morbidity across the globe. FmtA is a key factor linked with methicillin resistance in S. aureus. Consequently, new antibacterial compounds are crucial to combat S. aureus resistance. Here, we present the virtual screening of a set of compounds against the available crystal structure of FmtA. The findings indicate that gemifloxacin, paromomycin, streptomycin, and tobramycin were the top-ranked potential drug molecules based on the binding affinity. Furthermore, these drug molecules were analyzed with molecular dynamics simulations, which showed that the identified molecules formed highly stable FmtA–inhibitor(s) complexes. Molecular mechanics Poisson–Boltzmann surface area and quantum mechanics/molecular mechanics calculations suggested that the active site residues (Ser127, Lys130, Tyr211, and Asp213) of FmtA are crucial for the interaction with the inhibitor(s) to form stable protein–inhibitor(s) complexes. Moreover, fluorescence- and isothermal calorimetry-based binding studies showed that all the molecules possess dissociation constant values in the micromolar scale, revealing a strong binding affinity with FmtAΔ80, leading to stable protein–drug(s) complexes. The findings of this study present potential beginning points for the rational development of advanced, safe, and efficacious antibacterial agents targeting FmtA.

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Screening and Identification of Natural Product‐Like Compounds as Potential Antibacterial Agents Targeting FemC of Staphylococcus aureus: An in‐Silico Approach

Dalal

Kumari

2022

ChemistrySelect

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FemC is a methicillin resistance factor and regulates the synthesis of peptidoglycan in Staphylococcus aureus. Here, a set of natural product‐like compounds from Enamine and Selleckchem databases were screened at the active site of validated FemC model. Molecules that had interactions and good binding energies with protein were filtered by pharmacokinetic and ADMET properties. Molecular docking and molecular dynamics (MD) analysis displayed the identified molecules had stable and static interactions with FemC to form stable FemC‐inhibitor(s) complexes. Molecular Mechanics/Poisson‐Boltzmann Surface Area (MMPBSA) confirmed that identified molecules interacted with S15, M16, S17, R31, R43, Q47, K48, and R49 of FemC and resulted in the formation of lower energy complexes. The current study, hereby, reported the four (S4958 Glycocholic acid, SP‐146, Hupehenine, and Limonin) potent natural product‐like compounds that are required to be validated and may be further utilized to develop novel scaffolds for antimicrobials against S. aureus.

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Quantum Mechanics/Molecular Mechanics Studies on the Catalytic Mechanism of a Novel Esterase (FmtA) of Staphylococcus aureus

Cited by 31 publications

References 80 publications

Identification of a novel immune-inflammatory signature of COVID-19 infections, and evaluation of pharmacokinetics and therapeutic potential of RXn-02, a novel small-molecule derivative of quinolone

Identification of a novel immune-inflammatory signature of COVID-19 infections, and evaluation of pharmacokinetics and therapeutic potential of RXn-02, a novel small-molecule derivative of quinolone

Drug-Repurposing Approach To Combat Staphylococcus aureus: Biomolecular and Binding Interaction Study

Screening and Identification of Natural Product‐Like Compounds as Potential Antibacterial Agents Targeting FemC of Staphylococcus aureus: An in‐Silico Approach

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