2018
DOI: 10.3390/molecules23081899
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Binding Affinity via Docking: Fact and Fiction

Abstract: In 1982, Kuntz et al. published an article with the title “A Geometric Approach to Macromolecule-Ligand Interactions”, where they described a method “to explore geometrically feasible alignment of ligands and receptors of known structure”. Since then, small molecule docking has been employed as a fast way to estimate the binding pose of a given compound within a specific target protein and also to predict binding affinity. Remarkably, the first docking method suggested by Kuntz and colleagues aimed to predict … Show more

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Cited by 453 publications
(350 citation statements)
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References 73 publications
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“…Despite recent advances, molecular docking models often fail to accurately relate docking scores to experimental observables (e.g. binding affinity) due to methodological limitations such as the lack of active site dynamics, poorly described solvent interactions, and a crude description of hydrogen bonding [45]. However, the mu opioid regression model was able to correctly relate key modifications of the fentanyl core to experimentally measured binding affinity with r = 0.86 for eight congeners [1].…”
Section: Plos Onementioning
confidence: 99%
“…Despite recent advances, molecular docking models often fail to accurately relate docking scores to experimental observables (e.g. binding affinity) due to methodological limitations such as the lack of active site dynamics, poorly described solvent interactions, and a crude description of hydrogen bonding [45]. However, the mu opioid regression model was able to correctly relate key modifications of the fentanyl core to experimentally measured binding affinity with r = 0.86 for eight congeners [1].…”
Section: Plos Onementioning
confidence: 99%
“…[51] Hydrogen bond strength contributed significantly to increase binding affinity between protein and target molecules. [52] Unsubstituted compounds 1 a, 1 d, 3 a and 3 d were chosen for molecular docking interaction to demonstrate the effect of unsaturated keto exchange towards biological activity ( Table 1). S. aureus N-terminal domain of DNA binding protein (PDB entry: 4pql) was utilized as a receptor to evaluate the binding interaction with 1 a, 1 d, 3 a and 3 d.…”
Section: Molecular Dockingmentioning
confidence: 99%
“…The IC50 is not a direct indicator of affinity, although the indirectly related to confirm that NVP has more potency towards Hsp90 compared to RD. Entropy effects play an important role in drug-target interactions, but the entropic contribution to ligand-binding affinity is often omitted by endpoint binding free energy calculation methods such as MM/GBSA and MM/PBSA due to the high computational expense of normal mode analysis (NMA) [57,58]. The binding free energies estimated by including the truncated-NMA entropies based on the MD trajectories have been reported to give the lowest average absolute deviations against the experimental data among all the tested strategies for both MM/GBSA and MM/PBS [57,58].…”
Section: Mm/gbsa Binding Free Energy Calculationmentioning
confidence: 99%