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Vinylphosphonate-based cyclic dinucleotides enhance STING-mediated cancer immunotherapy

dc.contributor.authorDejmek, Milan
dc.contributor.authorBrázdová, Andrea
dc.contributor.authorOtava, Tomáš
dc.contributor.authorPimková Polidarová, Markéta
dc.contributor.authorKlima, Martin
dc.contributor.authorSmola, Miroslav
dc.contributor.authorVavřina, Zdeněk
dc.contributor.authorBuděšínský, Miloš
dc.contributor.authorDračínský, Martin
dc.contributor.authorLiboska, Radek
dc.contributor.authorBouřa, Evžen
dc.contributor.authorBirkuš, Gabriel
dc.contributor.authorNencka, Radim
dc.date.accessioned2023-09-26T11:40:29Z
dc.date.available2023-09-26T11:40:29Z
dc.date.issued2023
dc.identifier.urihttps://hdl.handle.net/20.500.14178/2031
dc.description.abstractCyclic dinucleotides (CDNs) trigger the cyclic GMP-AMP synthase-stimulator of interferon genes (cGAS-STING) pathway, which plays a key role in cytosolic DNA sensing and thus in immunomodulation against infections, cell damage and cancer. However, cancer immunotherapy trials with CDNs have shown immune activation, but not complete tumor regression. Nevertheless, we designed a novel class of CDNs containing vinylphosphonate based on a STING-affinity screening assay. In vitro, acyloxymethyl phosphate/phosphonate prodrugs of these vinylphosphonate CDNs were up to 1000-fold more potent than the clinical candidate ADU-S100. In vivo, the lead prodrug induced tumor-specific T cell priming and facilitated tumor regression in the 4T1 syngeneic mouse model of breast cancer. Moreover, we solved the crystal structure of this ligand bound to the STING protein. Therefore, our findings not only validate the therapeutic potential of vinylphosphonate CDNs but also open up opportunities for drug development in cancer immunotherapy bridging innate and adaptive immunity.en
dc.language.isoen
dc.relation.urlhttps://doi.org/10.1016/j.ejmech.2023.115685
dc.rightsCreative Commons Uveďte původ 4.0 Internationalcs
dc.rightsCreative Commons Attribution 4.0 Internationalen
dc.titleVinylphosphonate-based cyclic dinucleotides enhance STING-mediated cancer immunotherapyen
dcterms.accessRightsopenAccess
dcterms.licensehttps://creativecommons.org/licenses/by/4.0/legalcode
dc.date.updated2024-03-11T10:10:36Z
dc.subject.keywordcyclic dinucleotidesen
dc.subject.keywordSTINGen
dc.subject.keywordcanceren
dc.subject.keywordintratumoral administrationen
dc.subject.keywordimmunotherapyen
dc.relation.fundingReferenceinfo:eu-repo/grantAgreement/UK/COOP/COOP
dc.relation.fundingReferenceinfo:eu-repo/grantAgreement/MSM//LX22NPO5103
dc.relation.fundingReferenceinfo:eu-repo/grantAgreement/UK//SVV260691
dc.date.embargoStartDate2024-03-11
dc.type.obd73
dc.type.versioninfo:eu-repo/semantics/publishedVersion
dc.identifier.doi10.1016/j.ejmech.2023.115685
dc.identifier.utWos001059072400001
dc.identifier.eidScopus2-s2.0-85166974992
dc.identifier.obd636045
dc.identifier.pubmed37567057
dc.subject.rivPrimary30000::30100::30102
dc.subject.rivSecondary30000::30100
dc.subject.rivSecondary10000::10600::10608
dcterms.isPartOf.nameEuropean Journal of Medicinal Chemistry
dcterms.isPartOf.issn0223-5234
dcterms.isPartOf.journalYear2023
dcterms.isPartOf.journalVolume259
dcterms.isPartOf.journalIssueNovember
uk.faculty.primaryId115
uk.faculty.primaryNamePřírodovědecká fakultacs
uk.faculty.primaryNameFaculty of Scienceen
uk.department.primaryId1034
uk.department.primaryNameKatedra genetiky a mikrobiologiecs
uk.department.primaryNameDepartment of Genetics and Microbiologyen
uk.department.secondaryId1050
uk.department.secondaryId1048
uk.department.secondaryNameKatedra organické chemiecs
uk.department.secondaryNameDepartment of Organic Chemistryen
uk.department.secondaryNameKatedra biochemiecs
uk.department.secondaryNameDepartment of Biochemistryen
dc.type.obdHierarchyCsČLÁNEK V ČASOPISU::článek v časopisu::původní článekcs
dc.type.obdHierarchyEnJOURNAL ARTICLE::journal article::original articleen
dc.type.obdHierarchyCode73::152::206en
uk.displayTitleVinylphosphonate-based cyclic dinucleotides enhance STING-mediated cancer immunotherapyen


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