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dc.contributor.authorHoyos Nogués, Mireia
dc.contributor.authorFalgueras Batlle, Elena
dc.contributor.authorGinebra Molins, Maria Pau
dc.contributor.authorManero Planella, José María
dc.contributor.authorGil Mur, Francisco Javier
dc.contributor.authorMas Moruno, Carlos
dc.contributor.otherUniversitat Politècnica de Catalunya. Departament de Ciència i Enginyeria de Materials
dc.date.accessioned2020-01-29T18:05:44Z
dc.date.available2020-01-29T18:05:44Z
dc.date.issued2019-03-21
dc.identifier.citationHoyos, M. [et al.]. A dual molecular biointerface combining RGD and KRSR sequences improves osteoblastic functions by synergizing integrin and cell-membrane proteoglycan binding. "International journal of molecular sciences", 21 Març 2019, vol. 20, núm. 6, p. 1429:1-1429:13.
dc.identifier.issn1422-0067
dc.identifier.urihttp://hdl.handle.net/2117/176143
dc.description.abstractSynergizing integrin and cell-membrane heparan sulfate proteoglycan signaling on biomaterials through peptidic sequences is known to have beneficial effects in the attachment and behavior of osteoblasts; however, controlling the exact amount and ratio of peptides tethered on a surface is challenging. Here, we present a dual molecular-based biointerface combining integrin (RGD) and heparin (KRSR)-binding peptides in a chemically controlled fashion. To this end, a tailor-made synthetic platform (PLATF) was designed and synthesized by solid-phase methodologies. The PLATF and the control linear peptides (RGD or KRSR) were covalently bound to titanium via silanization. Physicochemical characterization by means of contact angle, Raman spectroscopy and XPS proved the successful and stable grafting of the molecules. The biological potential of the biointerfaces was measured with osteoblastic (Saos-2) cells both at short and long incubation periods. Biomolecule grafting (either the PLATF, RGD or KRSR) statistically improved (p < 0.05) cell attachment, spreading, proliferation and mineralization, compared to control titanium. Moreover, the molecular PLATF biointerface synergistically enhanced mineralization (p < 0.05) of Saos-2 cells compared to RGD or KRSR alone. These results indicate that dual-function coatings may serve to improve the bioactivity of medical implants by mimicking synergistic receptor binding.
dc.language.isoeng
dc.rightsCC BY 4.0
dc.rights.urihttp://creativecommons.org/licenses/by-nc-nd/3.0/es/
dc.subjectÀrees temàtiques de la UPC::Enginyeria biomèdica::Biomaterials
dc.subject.lcshBiomedical materials
dc.subject.otherBiointerface
dc.subject.otherTitanium
dc.subject.otherFunctionalization
dc.subject.otherRGD
dc.subject.otherIntegrin
dc.subject.otherKRSR
dc.subject.otherProteoglycan
dc.subject.otherOsteointegration
dc.subject.otherOsteoblast
dc.subject.otherCoating
dc.titleA dual molecular biointerface combining RGD and KRSR sequences improves osteoblastic functions by synergizing integrin and cell-membrane proteoglycan binding
dc.typeArticle
dc.subject.lemacMaterials biomèdics
dc.subject.lemacTitani
dc.contributor.groupUniversitat Politècnica de Catalunya. BBT - Biomaterials, Biomecànica i Enginyeria de Teixits
dc.contributor.groupUniversitat Politècnica de Catalunya. CRnE - Centre de Recerca en Ciència i Enginyeria Multiescala de Barcelona
dc.identifier.doi10.3390/ijms20061429
dc.relation.publisherversionhttps://www.mdpi.com/1422-0067/20/6/1429
dc.rights.accessOpen Access
local.identifier.drac24239563
dc.description.versionPostprint (published version)
dc.relation.projectidinfo:eu-repo/grantAgreement/MINECO//MAT2015-67183-R/ES/RECUBRIMIENTOS OSTEOINDUCTIVOS Y ANTIMICROBIANOS AVANZADOS PARA MEJORAR LA OSTEOINTEGRACION DE BIOMATERIALES EN PATOLOGIAS OSTEOPOROTICAS Y DIABETICAS/
dc.relation.projectidinfo:eu-repo/grantAgreement/AEI/Plan Estatal de Investigación Científica y Técnica y de Innovación 2013-2016/MAT2017-83905-R/ES/SUPERFICIES MULTIFUNCIONALES BIOMIMETICAS: UNA NUEVA ESTRATEGIA BIOMOLECULAR PARA CONTROLAR LA RESPUESTA CELULAR EN TERAPIAS REGENERATIVAS/
dc.contributor.covenanteeUniversitat Internacional de Catalunya
local.citation.authorHoyos, M.; Falgueras, E.; Ginebra, M.P.; Manero, J.; Gil, F.J.; Mas-Moruno, C.
local.citation.publicationNameInternational journal of molecular sciences
local.citation.volume20
local.citation.number6
local.citation.startingPage1429:1
local.citation.endingPage1429:13


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