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An evaluation of indirubin analogues as phosphorylase kinase inhibitors

dc.creatorBegum, J.en
dc.creatorSkamnaki, V. T.en
dc.creatorMoffatt, C.en
dc.creatorBischler, N.en
dc.creatorSarrou, J.en
dc.creatorSkaltsounis, A. L.en
dc.creatorLeonidas, D. D.en
dc.creatorOikonomakos, N. G.en
dc.creatorHayes, J. M.en
dc.date.accessioned2015-11-23T10:23:43Z
dc.date.available2015-11-23T10:23:43Z
dc.date.issued2015
dc.identifier10.1016/j.jmgm.2015.07.010
dc.identifier.issn10933263
dc.identifier.urihttp://hdl.handle.net/11615/26224
dc.description.abstractPhosphorylase kinase (PhK) has been linked with a number of conditions such as glycogen storage diseases, psoriasis, type 2 diabetes and more recently, cancer (Camus et al., 2012 [6]). However, with few reported structural studies on PhK inhibitors, this hinders a structure based drug design approach. In this study, the inhibitory potential of 38 indirubin analogues have been investigated. 11 of these ligands had IC<inf>50</inf> values in the range 0.170-0.360 μM, with indirubin-3′-acetoxime (1c) the most potent. 7-Bromoindirubin-3′-oxime (13b), an antitumor compound which induces caspase-independent cell-death (Ribas et al., 2006 [20]) is revealed as a specific inhibitor of PhK (IC<inf>50</inf> = 1.8 μM). Binding assay experiments performed using both PhK-holo and PhK-γtrnc confirmed the inhibitory effects to arise from binding at the kinase domain (γ subunit). High level computations using QM/MM-PBSA binding free energy calculations were in good agreement with experimental binding data, as determined using statistical analysis, and support binding at the ATP-binding site. The value of a QM description for the binding of halogenated ligands exhibiting σ-hole effects is highlighted. A new statistical metric, the 'sum of the modified logarithm of ranks' (SMLR), has been defined which measures performance of a model for both the "early recognition" (ranking earlier/higher) of active compounds and their relative ordering by potency. Through a detailed structure activity relationship analysis considering other kinases (CDK2, CDK5 and GSK-3α/β), 6′(Z) and 7(L) indirubin substitutions have been identified to achieve selective PhK inhibition. The key PhK binding site residues involved can also be targeted using other ligand scaffolds in future work. © 2015 Elsevier Inc.en
dc.sourceJournal of Molecular Graphics and Modellingen
dc.source.urihttp://www.scopus.com/inward/record.url?eid=2-s2.0-84941356336&partnerID=40&md5=51ed5efc9cec0be0c2b69e5cd32be482
dc.subjectGlycogen phosphorylaseaen
dc.subjectIndirubinsen
dc.subjectKinase inhibitorsen
dc.subjectQM/MM-PBSAen
dc.subjectSigma-holeen
dc.subjectType 2 diabetesen
dc.subjectCell deathen
dc.subjectDigital storageen
dc.subjectEnzyme activityen
dc.subjectEnzyme inhibitionen
dc.subjectEnzymesen
dc.subjectFree energyen
dc.subjectLigandsen
dc.subjectPhosphorylationen
dc.subjectType-2 diabetesen
dc.subjectBinding energyen
dc.subject6 bromo 5 methylindirubinen
dc.subject6 bromo 5 methylindirubin 3' acetoximeen
dc.subject6 bromo 5 nitroindirubin 3' acetoximeen
dc.subject6 bromo 5 nitroindirubin 3' oximeen
dc.subject6 bromo n methylindirubinen
dc.subject6 bromo n methylindirubin 3' acetoximeen
dc.subject6 bromoindirubinen
dc.subject6 bromoindirubin 3' acetoximeen
dc.subject6 bromoindirubin 3' oximeen
dc.subject6 chloroindirubinen
dc.subject6 chloroindirubin 3' oximeen
dc.subject6 fluoroindirubinen
dc.subject6 fluoroindirubin 3' oximeen
dc.subject6 iodoindirubin 3' oximeen
dc.subject6 Methoxindirubin 3' acetoximeen
dc.subject6 Methoxindirubin 3' oximeen
dc.subject6 vinylindirubinen
dc.subject6 vinylindirubin 3' acetoximeen
dc.subject6 vinylindirubin 3' oximeen
dc.subject6,5 dichloroindirubin 3' acetoximeen
dc.subject6,5 dichloroindirubin 3' oximeen
dc.subject6,6 dibromoindirubin 3' oximeen
dc.subject7 bromoindirubin 3' acetoximeen
dc.subject7 bromoindirubin 3' oximeen
dc.subjectantineoplastic agenten
dc.subjectindirubinen
dc.subjectindirubin 3' acetoximeen
dc.subjectindirubin 3' methoximeen
dc.subjectindirubin 3' oximeen
dc.subjectunclassified drugen
dc.subjectunindexed drugen
dc.subjectanimal tissueen
dc.subjectantineoplastic activityen
dc.subjectArticleen
dc.subjectbinding affinityen
dc.subjectbinding siteen
dc.subjectdrug potencyen
dc.subjectdrug screeningen
dc.subjectdrug selectivityen
dc.subjectfemaleen
dc.subjectmolecular dockingen
dc.subjectmolecular mechanicsen
dc.subjectnonhumanen
dc.subjectpriority journalen
dc.subjectquantum mechanicsen
dc.subjectrabbiten
dc.subjectstructure activity relationen
dc.titleAn evaluation of indirubin analogues as phosphorylase kinase inhibitorsen
dc.typejournalArticleen


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