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Development of a Nucleotide Exchange Inhibitor That Impairs Ras Oncogenic Signaling

dc.contributor.authorMarín Ramos, Nagore Isasbel
dc.contributor.authorPiñar Pinedo, María del Carmen
dc.contributor.authorVázquez Villa, María Del Henar
dc.contributor.authorMartín-Fontecha Corrales, María Del Mar
dc.contributor.authorGonzalez Wong, Ángel
dc.contributor.authorCanales Mayordomo, María Ángeles
dc.contributor.authorAlgar Lizana, Sergio
dc.contributor.authorMayo Mariscal de Gante, Paloma P.
dc.contributor.authorJiménez-Barbero, Jesús
dc.contributor.authorGajate Fraile, Consuelo
dc.contributor.authorMollinedo García, Faustino
dc.contributor.authorPardo Carrasco, Leonardo
dc.contributor.authorOrtega Gutiérrez, Silvia
dc.contributor.authorViso Beronda, Alma
dc.contributor.authorLópez Rodríguez, María Luz
dc.date.accessioned2023-06-17T22:15:45Z
dc.date.available2023-06-17T22:15:45Z
dc.date.issued2017-01-31
dc.descriptionManuscript Received: 20 October 2016; Accepted manuscript online: 25 November 2016; Version of record online: 27 December 2016; Issue online: 1 February 2017
dc.description.abstractDespite more than three decades of intense effort, no anti-Ras therapies have reached clinical application. Contributing to this failure has been an underestimation of Ras complexity and a dearth of structural information. In this regard, recent studies have revealed the highly dynamic character of the Ras surface and the existence of transient pockets suitable for small-molecule binding, opening up new possibilities for the development of Ras modulators. Herein, a novel Ras inhibitor (compound 12) is described that selectively impairs mutated Ras activity in a reversible manner without significantly affecting wild-type Ras, reduces the Ras–guanosine triphosphate (GTP) levels, inhibits the activation of the mitogen-activated protein kinase (MAPK) pathway, and exhibits remarkable cytotoxic activity in Ras-driven cellular models. The use of molecular dynamics simulations and NMR spectroscopy experiments has enabled the molecular bases responsible for the interactions between compound 12 and Ras protein to be explored. The new Ras inhibitor binds partially to the GTP-binding region and extends into the adjacent hydrophobic pocket delimited by switch II. Hence, Ras inhibitor 12 could represent a new compound for the development of more efficacious drugs to target Ras-driven cancers; a currently unmet clinical need.
dc.description.departmentSección Deptal. de Química Orgánica (Óptica y Optometría)
dc.description.facultyFac. de Óptica y Optometría
dc.description.refereedTRUE
dc.description.sponsorshipMinisterio de Economía y Competitividad (MINECO)
dc.description.sponsorshipComunidad de Madrid
dc.description.statuspub
dc.eprint.idhttps://eprints.ucm.es/id/eprint/45837
dc.identifier.doi10.1002/chem.201604905
dc.identifier.issn0947-6539
dc.identifier.officialurlhttp://dx.doi.org/10.1002/chem.201604905
dc.identifier.urihttps://hdl.handle.net/20.500.14352/18289
dc.issue.number7
dc.journal.titleChemistry: a european journal
dc.language.isoeng
dc.page.final1685
dc.page.initial1676
dc.publisherWiley
dc.relation.projectIDSAF2016-78792-R
dc.relation.projectIDSAF2013-48271-R
dc.relation.projectIDSAF2014-59716-R
dc.relation.projectID(S2010/BMD-2353)
dc.rights.accessRightsrestricted access
dc.subject.cdu577.112
dc.subject.cdu616-006.04
dc.subject.cdu612.398
dc.subject.keywordCancer
dc.subject.keywordDrug design
dc.subject.keywordInhibitors
dc.subject.keywordMedicinal chemistry
dc.subject.keywordProteins
dc.subject.ucmBioquímica (Medicina)
dc.subject.ucmOncología
dc.subject.unesco3201.01 Oncología
dc.titleDevelopment of a Nucleotide Exchange Inhibitor That Impairs Ras Oncogenic Signaling
dc.typejournal article
dc.volume.number23
dspace.entity.typePublication
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relation.isAuthorOfPublication.latestForDiscovery5abc3db9-c8c9-485b-81f6-2e2d663e9982

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