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Glucose-based spiro-isoxazolines: A new family of potent glycogen phosphorylase inhibitors

dc.contributor.authorBenltifa, Mahmouden
dc.contributor.authorHayes, Joseph M.en
dc.contributor.authorVidal, Sébastienen
dc.contributor.authorGueyrard, Daviden
dc.contributor.authorGoekjian, Peter G.en
dc.contributor.authorPraly, Jean Pierreen
dc.contributor.authorKizilis, Gregoryen
dc.contributor.authorTiraidis, Costasen
dc.contributor.authorAlexacou, Kyra Melindaen
dc.contributor.authorChrysina, Evangelia D.en
dc.contributor.authorZographos, Spyros E.en
dc.contributor.authorLeonidas, Demetres D.en
dc.contributor.authorArchontis, Georgios Z.en
dc.contributor.authorOikonomakos, Nikos G.en
dc.creatorBenltifa, Mahmouden
dc.creatorHayes, Joseph M.en
dc.creatorVidal, Sébastienen
dc.creatorGueyrard, Daviden
dc.creatorGoekjian, Peter G.en
dc.creatorPraly, Jean Pierreen
dc.creatorKizilis, Gregoryen
dc.creatorTiraidis, Costasen
dc.creatorAlexacou, Kyra Melindaen
dc.creatorChrysina, Evangelia D.en
dc.creatorZographos, Spyros E.en
dc.creatorLeonidas, Demetres D.en
dc.creatorArchontis, Georgios Z.en
dc.creatorOikonomakos, Nikos G.en
dc.date.accessioned2019-12-02T15:28:45Z
dc.date.available2019-12-02T15:28:45Z
dc.date.issued2009
dc.identifier.urihttp://gnosis.library.ucy.ac.cy/handle/7/58530
dc.description.abstractA series of glucopyranosylidene-spiro-isoxazolines was prepared through regio- and stereoselective [3+2]-cycloaddition between the methylene acetylated exo-glucal and aromatic nitrile oxides. The deprotected cycloadducts were evaluated as inhibitors of muscle glycogen phosphorylase b. The carbohydrate-based family of five inhibitors displays Ki values ranging from 0.63 to 92.5 μM. The X-ray structures of the enzyme-ligand complexes show that the inhibitors bind preferentially at the catalytic site of the enzyme retaining the less active T-state conformation. Docking calculations with GLIDE in extra-precision (XP) mode yielded excellent agreement with experiment, as judged by comparison of the predicted binding modes of the five ligands with the crystallographic conformations and the good correlation between the docking scores and the experimental free binding energies. Use of docking constraints on the well-defined positions of the glucopyranose moiety in the catalytic site and redocking of GLIDE-XP poses using electrostatic potential fit-determined ligand partial charges in quantum polarized ligand docking (QPLD) produced the best results in this regard. © 2009 Elsevier Ltd. All rights reserved.en
dc.sourceBioorganic and Medicinal Chemistryen
dc.source.urihttps://www.scopus.com/inward/record.uri?eid=2-s2.0-71249106036&doi=10.1016%2fj.bmc.2009.08.060&partnerID=40&md5=e4fc9f93037cab15d8a8b255acdb47e8
dc.subjectarticleen
dc.subjectunclassified drugen
dc.subjectdrug activityen
dc.subjectOxazolesen
dc.subjectEnzyme Inhibitorsen
dc.subjectKineticsen
dc.subjectenzyme inhibitionen
dc.subjectMagnetic Resonance Spectroscopyen
dc.subjectX ray crystallographyen
dc.subjectmolecular dockingen
dc.subjectSpectrometry, Mass, Electrospray Ionizationen
dc.subjectModels, Molecularen
dc.subjectCrystallography, X-Rayen
dc.subjectstereochemistryen
dc.subjectcycloadditionen
dc.subjectenzyme inhibitoren
dc.subjectGlucoseen
dc.subjectglucose derivativeen
dc.subjectGlycogen phosphorylaseen
dc.subjectX-ray crystallographyen
dc.subjectglycogen phosphorylase inhibitoren
dc.subject1,3-Dipolar cycloadditionen
dc.subjectdrug conformationen
dc.subjectenzyme inhibitor complexen
dc.subjectGLIDE docking calculationsen
dc.subjectIsoxazolineen
dc.subjectisoxazoline derivativeen
dc.subjectQuantum polarized ligand docking (QPLD)en
dc.titleGlucose-based spiro-isoxazolines: A new family of potent glycogen phosphorylase inhibitorsen
dc.typeinfo:eu-repo/semantics/article
dc.identifier.doi10.1016/j.bmc.2009.08.060
dc.description.volume17
dc.description.issue20
dc.description.startingpage7368
dc.description.endingpage7380
dc.author.facultyΣχολή Θετικών και Εφαρμοσμένων Επιστημών / Faculty of Pure and Applied Sciences
dc.author.departmentΤμήμα Φυσικής / Department of Physics
dc.type.uhtypeArticleen
dc.description.notes<p>Cited By :48</p>en
dc.source.abbreviationBioorg.Med.Chem.en
dc.contributor.orcidChrysina, Evangelia D. [0000-0001-8147-9030]
dc.contributor.orcidZographos, Spyros E. [0000-0001-8455-2352]
dc.contributor.orcidLeonidas, Demetres D. [0000-0002-3874-2523]
dc.contributor.orcidArchontis, Georgios Z. [0000-0002-7750-8641]
dc.gnosis.orcid0000-0001-8147-9030
dc.gnosis.orcid0000-0001-8455-2352
dc.gnosis.orcid0000-0002-3874-2523
dc.gnosis.orcid0000-0002-7750-8641


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