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dc.contributor.authorHealy, Fiona M.
dc.contributor.authorTurner, Amy L.
dc.contributor.authorMarensi, Vanessa
dc.contributor.authorMacEwan, David
dc.date.accessioned2024-10-04T09:57:15Z
dc.date.available2024-10-04T09:57:15Z
dc.date.issued2024-09-20
dc.date.submitted2024-05-31
dc.identifierhttps://chesterrep.openrepository.com/bitstream/handle/10034/629064/fphar-15-1441938.pdf?sequence=3
dc.identifier.citationHealy, F. M., Turner, A. L., Marensi, V., & MacEwan, D. (2024). Mediating kinase activity in Ras-mutant cancer: Potential for an individualised approach? Frontiers in Pharmacology, 15, article-number 1441938. https://doi.org/10.3389/fphar.2024.1441938en_US
dc.identifier.doi10.3389/fphar.2024.1441938en_US
dc.identifier.urihttp://hdl.handle.net/10034/629064
dc.descriptionCopyright © 2024 Healy, Turner, Marensi and MacEwanen_US
dc.description.abstractIt is widely acknowledged that there is a considerable number of oncogenic mutations within the Ras superfamily of small GTPases which are the driving force behind a multitude of cancers. Ras proteins mediate a plethora of kinase pathways, including the MAPK, PI3K, and Ral pathways. Since Ras was considered undruggable until recently, pharmacological targeting of pathways downstream of Ras has been attempted to varying success, though drug resistance has often proven an issue. Nuances between kinase pathway activation in the presence of various Ras mutants are thought to contribute to the resistance, however, the reasoning behind activation of different pathways in different Ras mutational contexts is yet to be fully elucidated. Indeed, such disparities often depend on cancer type and disease progression. However, we are in a revolutionary age of Ras mutant targeted therapy, with direct-targeting KRAS-G12C inhibitors revolutionising the field and achieving FDA-approval in recent years. However, these are only beneficial in a subset of patients. Approximately 90% of Ras-mutant cancers are not KRAS-G12C mutant, and therefore raises the question as to whether other distinct amino acid substitutions within Ras may one day be targetable in a similar manner, and indeed whether better understanding of the downstream pathways these various mutants activate could further improve therapy. Here, we discuss the favouring of kinase pathways across an array of Ras-mutant oncogenic contexts and assess recent advances in pharmacological targeting of various Ras mutants. Ultimately, we will examine the utility of individualised pharmacological approaches to Ras-mediated cancer.en_US
dc.description.sponsorshipUnfundeden_US
dc.languageen
dc.publisherFrontiers Mediaen_US
dc.relation.urlhttps://www.frontiersin.org/journals/pharmacology/articles/10.3389/fphar.2024.1441938/fullen_US
dc.rightsLicence for this article: http://creativecommons.org/licenses/by/4.0/
dc.rights.urihttps://creativecommons.org/licenses/by/4.0/en_US
dc.sourceeissn: 1663-9812
dc.subjecttargeted therapyen_US
dc.subjectkinaseen_US
dc.subjectsignallingen_US
dc.subjectRasen_US
dc.subjectmutationen_US
dc.subjectcanceren_US
dc.titleMediating Kinase Activity in Ras-Mutant Cancer: Potential for an Individualised Approach?en_US
dc.typeArticleen_US
dc.identifier.eissn1663-9812en_US
dc.contributor.departmentUniversity of Liverpool; University of Chesteren_US
dc.identifier.journalFrontiers in Pharmacologyen_US
dc.date.updated2024-10-04T08:10:16Z
dc.date.accepted2024-09-06
rioxxterms.identifier.projectUnfundeden_US
rioxxterms.versionVoRen_US
dc.date.deposited2024-10-04en_US


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