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dc.contributor.authorRamos Valle, Andrés
dc.contributor.authorDomínguez, Arnau
dc.contributor.authorNavarro, Natalia
dc.contributor.authorMárquez López, Ana
dc.contributor.authorAviñó, Anna
dc.contributor.authorEritja, Ramón
dc.contributor.authorFàbrega, Carme
dc.contributor.authorGarcía Hevia, Lorena 
dc.contributor.authorLópez Fanarraga, Mónica 
dc.contributor.otherUniversidad de Cantabriaes_ES
dc.date.accessioned2025-07-08T09:10:35Z
dc.date.issued2025
dc.identifier.issn1613-6810
dc.identifier.issn1613-6829
dc.identifier.otherTED2021-129248Be100es_ES
dc.identifier.otherTED2021-129248B-100es_ES
dc.identifier.otherPID2020-118145RB-I00es_ES
dc.identifier.urihttps://hdl.handle.net/10902/36619
dc.description.abstractMalignant melanoma presents a significant challenge in oncology due to its aggressive nature and high metastatic potential. Conventional systemic treatments often fail to effectively reach tumor sites, limiting their therapeutic impact. This study introduces a groundbreaking triple-strategy approach for treating malignant melanoma. A novel prodrug, an oligonucleotide, comprising 10 units of Floxuridine (5-fluoro-2'-deoxyuridine) (FdU) nucleoside antimetabolites are developed, to enhance half-life and reduce rapid metabolism. Encapsulated in soluble colloidal silica nanoparticles, this compound is protected and directed toward tumor neovasculature precursor endothelial cell receptors, ensuring local delivery. The strategy focuses on releasing the prodrug in the tumor microenvironment, aiming to eradicate both melanoma cells and their supportive structures. Efficacy is demonstrated in cell culture studies and preclinical models of malignant melanoma, showing a remarkable 50% reduction in tumor size after just three intravenous treatments. These findings underscore the transformative potential of targeting endothelial cell membrane proteins for drug delivery. This study paves the way for innovative targeted therapies, promising significant advancements in treatment strategies and improves outcomes for patients with metastatic cancers.es_ES
dc.description.sponsorshipWe acknowledge the financial support from the Spanish Instituto de Salud Carlos III, under Project ref. DTS24/000237, PI22/00030, and PI23/00261 co-funded by the European Regional Development Fund, “Investing in your future,” Grant TED2021-129248 BeI00 the Spanish Ministerio de Ciencia e Innovación (MICINN) Projects PID2020-118145RB-I00 and TED2021-129248B-100, co-funded by the European Union FEDER funds; the Gobierno Regional de Cantabria and IDIVAL for the project Refs INNVAL21/19, NEXTVAL 22/12, and AR IDI-020-022 fellowship; N.N. held a predoctoral contract grant (PRE2021-097856). We also thank Oligonucleotide synthesis was performed by the ICTS ‘‘NANBIOSIS” (CIBER BBN) and specifically by the https://www.nanbiosis.es/portfolio/u29-oligonucleotide-synthesis-platform-osp/ oligonucleotide synthesis platform (OSP) U29 at IQAC-CSIC.es_ES
dc.format.extent12 p.es_ES
dc.language.isoenges_ES
dc.publisherWiley-VCH Verlages_ES
dc.rights© Wiley-VCH Verlages_ES
dc.sourceSmall, 2025, 21(20), 2407752es_ES
dc.subject.otherMalignant melanomaes_ES
dc.subject.otherVEGF receptores_ES
dc.subject.otherTEM8es_ES
dc.subject.otherTherapeutic oligonucleotidees_ES
dc.subject.otherSilica nanoparticleses_ES
dc.subject.otherTargeted deliveryes_ES
dc.subject.otherTumor neovasculaturees_ES
dc.titleTargeted tumor microenvironment delivery of floxuridine prodrug via soluble silica nanoparticles in malignant melanoma as a model for aggressive cancer treatmentes_ES
dc.typeinfo:eu-repo/semantics/articlees_ES
dc.relation.publisherVersionhttps://doi.org/10.1002/smll.202407752es_ES
dc.rights.accessRightsembargoedAccesses_ES
dc.relation.projectIDinfo:eu-repo/grantAgreement/AEI/Plan Estatal de Investigación Científica y Técnica y de Innovación 2017-2020/PID2020-118145RB-I00/ES/ESTRUCTURAS DE ADN Y SISTEMAS DE ADMINISTRACION DE MEDICAMENTOS/es_ES
dc.identifier.DOI10.1002/smll.202407752
dc.type.versionacceptedVersiones_ES
dc.embargo.lift2026-05-01
dc.date.embargoEndDate2026-05-01


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