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dc.contributor.authorLee, Y.
dc.contributor.authorKim, S.
dc.contributor.authorKim, J.
dc.contributor.authorArooj, Mahreen
dc.contributor.authorKim, S.
dc.contributor.authorHwang, S.
dc.contributor.authorKim, B.
dc.contributor.authorPark, K.
dc.contributor.authorLee, K.
dc.date.accessioned2017-01-30T10:37:14Z
dc.date.available2017-01-30T10:37:14Z
dc.date.created2015-10-29T04:08:41Z
dc.date.issued2014
dc.identifier.citationLee, Y. and Kim, S. and Kim, J. and Arooj, M. and Kim, S. and Hwang, S. and Kim, B. et al. 2014. Binding mode analyses and pharmacophore model development for stilbene derivatives as a novel and competitive class of α-glucosidase inhibitors. PLoS ONE. 9 (1).
dc.identifier.urihttp://hdl.handle.net/20.500.11937/4196
dc.identifier.doi10.1371/journal.pone.0085827
dc.description.abstract

Stilbene urea derivatives as a novel and competitive class of non-glycosidic α-glucosidase inhibitors are effective for the treatment of type II diabetes and obesity. The main purposes of our molecular modeling study are to explore the most suitable binding poses of stilbene derivatives with analyzing the binding affinity differences and finally to develop a pharmacophore model which would represents critical features responsible for α-glucosidase inhibitory activity. Three-dimensional structure of S. cerevisiae α-glucosidase was built by homology modeling method and the structure was used for the molecular docking study to find out the initial binding mode of compound 12, which is the most highly active one. The initial structure was subjected to molecular dynamics (MD) simulations for protein structure adjustment at compound 12-bound state. Based on the adjusted conformation, the more reasonable binding modes of the stilbene urea derivatives were obtained from molecular docking and MD simulations. The binding mode of the derivatives was validated by correlation analysis between experimental Ki value and interaction energy. Our results revealed that the binding modes of the potent inhibitors were engaged with important hydrogen bond, hydrophobic, and π-interactions. With the validated compound 12-bound structure obtained from combining approach of docking and MD simulation, a proper four featured pharmacophore model was generated. It was also validated by comparison of fit values with the Ki values. Thus, these results will be helpful for understanding the relationship between binding mode and bioactivity and for designing better inhibitors from stilbene derivatives.

dc.publisherPublic Library of Science
dc.titleBinding mode analyses and pharmacophore model development for stilbene derivatives as a novel and competitive class of α-glucosidase inhibitors
dc.typeJournal Article
dcterms.source.volume9
dcterms.source.number1
dcterms.source.titlePLoS ONE
curtin.note

This open access article is distributed under the Creative Commons license http://creativecommons.org/licenses/by/4.0/

curtin.departmentSchool of Biomedical Sciences
curtin.accessStatusOpen access


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