2019
DOI: 10.1080/10799893.2019.1605528
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An explorative study on Staphylococcus aureus MurE inhibitor: induced fit docking, binding free energy calculation, and molecular dynamics

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Cited by 6 publications
(4 citation statements)
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“…S. aureus is an important human pathogen and is among the leading causes of skin and soft tissue and device-related infections, as well as infective endocarditis. The S. aureus MurE enzyme is one of the potential targets for the development of new therapeutic agents due to its high substrate specificity and ubiquitous nature among bacteria ( Azam, Saha & Jupudi, 2019 ). The residues and binding types where both ligands bind to the active binding site of the S. aureus receptor are also shown in Fig.…”
Section: Resultsmentioning
confidence: 99%
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“…S. aureus is an important human pathogen and is among the leading causes of skin and soft tissue and device-related infections, as well as infective endocarditis. The S. aureus MurE enzyme is one of the potential targets for the development of new therapeutic agents due to its high substrate specificity and ubiquitous nature among bacteria ( Azam, Saha & Jupudi, 2019 ). The residues and binding types where both ligands bind to the active binding site of the S. aureus receptor are also shown in Fig.…”
Section: Resultsmentioning
confidence: 99%
“…Three hydroxyl groups and one oxygen atom in quercetin were connected to the residues (ASP207, ASN151, LYS114, and ARG187) at the active binding site via hydrogen bonds (2.03, 2.71, 2.12, 2.14 and 2.20 Å), as shown in Table S1 . In a study on the Staphylococcus aureus MurE inhibitor, it was observed that the molecule whose inhibitory activity was investigated provides this activity by making hydrogen bonds with the active binding site of the similar residues with ASN151, THR152, SER180, ARG187 AND LYS219 ( Azam, Saha & Jupudi, 2019 ). These hydrogen bonding interactions are considered important interactions for the stabilization of the inhibitor within the catalytic pocket of S. aureus MurE.…”
Section: Resultsmentioning
confidence: 99%
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“…For inhibition of the CYP450, as it is implied from the physics of the problem, the free energy of solvation of drug candidates in different solvents can determine the free energy of docking the drugs to the active site of the enzyme [64,65]. To that end, the most widely considered solvents are octanol and water, commonly employed as octanol-water partition coefficient [66][67][68][69][70].…”
Section: Analysis Of the Performance Of Studied Solvents And Representationsmentioning
confidence: 99%