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dc.contributor.authorRADOMSKI, MAREKen
dc.contributor.authorMEDINA MARTIN, CARLOSen
dc.date.accessioned2015-01-14T14:25:13Z
dc.date.available2015-01-14T14:25:13Z
dc.date.issued2013en
dc.date.submitted2013en
dc.identifier.citationWang, J., Radomski, M.W., Medina, C., Gilmer, J.F, MMP inhibition by barbiturate homodimers, Bioorganic and Medicinal Chemistry Letters, 23, 2013, 444 - 447en
dc.identifier.otherYen
dc.descriptionPUBLISHEDen
dc.description.abstractWe have studied some homodimeric compounds derived from 5-homopiperazine substituted pyrimidine triones (barbiturates) with linkers in the range 2-20 carbon atoms. The compounds were designed to be capable of resisting absorption, to be stable in the gut and to maintain inhibitory potency against gelatinases and related function. The compounds were then assessed for inhibitory potency against a panel of MMPs (1, 2, 8, 9 and 13). The dimer compounds had similar potency and selectivity to the homopiperazine barbiturate monomer class. At 100 nM, selected dimers significantly inhibited cancer cell invasion in a matrigel assay using Caco-2 cells stimulated by hepatic growth factor. Finally, selected dimers showed adequate stability in simulated intestinal fluid to suggest the capacity to transit to the colon.en
dc.format.extent444en
dc.format.extent447en
dc.language.isoenen
dc.relation.ispartofseriesBioorganic and Medicinal Chemistry Lettersen
dc.relation.ispartofseries23en
dc.rightsYen
dc.subjectPharmacyen
dc.titleMMP inhibition by barbiturate homodimersen
dc.typeJournal Articleen
dc.type.supercollectionscholarly_publicationsen
dc.type.supercollectionrefereed_publicationsen
dc.identifier.peoplefinderurlhttp://people.tcd.ie/radomskmen
dc.identifier.peoplefinderurlhttp://people.tcd.ie/martinc2en
dc.identifier.rssinternalid82921en
dc.rights.ecaccessrightsopenAccess
dc.subject.TCDThemeCanceren
dc.identifier.urihttp://hdl.handle.net/2262/72997


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