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dc.contributor.author GIBBENS BANDALA, BRENDA VIANEY
dc.contributor.author MORALES AVILA, ENRIQUE
dc.contributor.author FERRO FLORES, GUILLERMINA
dc.contributor.author SANTOS CUEVAS, CLARA LETICIA
dc.contributor.author LUNA GUTIERREZ, MYRNA ALEJANDRA
dc.contributor.author RAMIREZ NAVA, GERARDO JULIAN
dc.contributor.author OCAMPO GARCIA, BLANCA ELI
dc.creator GIBBENS BANDALA, BRENDA VIANEY; 450667
dc.creator MORALES AVILA, ENRIQUE; 170668
dc.creator FERRO FLORES, GUILLERMINA; 19581
dc.creator SANTOS CUEVAS, CLARA LETICIA; 171596
dc.creator LUNA GUTIERREZ, MYRNA ALEJANDRA; 265081
dc.creator RAMIREZ NAVA, GERARDO JULIAN; 646758
dc.creator OCAMPO GARCIA, BLANCA ELI; 309879
dc.date.accessioned 2020-01-22T20:52:36Z
dc.date.available 2020-01-22T20:52:36Z
dc.date.issued 2019-09-27
dc.identifier.issn 2073-4360
dc.identifier.uri http://hdl.handle.net/20.500.11799/105354
dc.description.abstract The peptide-receptor radionuclide therapy (PRRT) is a successful approach for selectively delivering radiation within tumor sites through specific recognition of radiolabeled peptides by overexpressed receptors on cancer cell surfaces. The e cacy of PRRT could be improved by using polymeric radio- and drug- therapy nanoparticles for a concomitant therapeutic e ect on malignant cells. This research aimed to prepare and evaluate, a novel drug and radiation delivery nanosystem based on the 177Lu-labeled polyamidoamine (PAMAM) dendrimer (DN) loaded with paclitaxel (PTX) and functionalized on the surface with the Lys1Lys3(DOTA)-bombesin (BN) peptide for specific targeting to gastrin-releasing peptide receptors (GRPr) overexpressed on breast cancer cells. DN was first conjugated covalently to BN and DOTA (chemical moiety for lutetium-177 complexing) and subsequently loaded with PTX. The characterization by microscopic and spectroscopic techniques, in-vitro drug delivery tests as well as in in-vitro and in-vivo cellular uptake of 177Lu-DOTA-DN(PTX)-BN by T47D breast cancer cells (GRPr-positive), indicated the formation of an improved delivery nanosystem with target-specific recognition by GRPr. Results of the 177Lu-DOTA-DN(PTX)-BN e ect on T47D cell viability (1.3%, compared with 10.9% of 177Lu-DOTA-DN-BN and 14.0% of DOTA-DN-(PTX)-BN) demonstrated the concomitant radiotherapeutic and chemotherapeutic properties of the polymeric nanosystem as a potential agent for the treatment of GRPr-positive tumors. es
dc.description.sponsorship This study was supported by the grant CONACyT-CB-A1S38087 and the International Atomic Energy Agency (CRP-F2264). It was performed as part of the activities of the “Laboratorio Nacional de Investigación y Desarrollo de Radiofármacos, CONACyT”. es
dc.language.iso eng es
dc.publisher Polymers, MDPI es
dc.rights openAccess es
dc.rights.uri http://creativecommons.org/licenses/by-nc-nd/4.0
dc.subject polymeric nanosystems es
dc.subject dendrimers es
dc.subject radiotherapy es
dc.subject GRPr es
dc.subject paclitaxel es
dc.subject lutetium-177 es
dc.subject.classification BIOLOGÍA Y QUÍMICA
dc.title Synthesis and Evaluation of 177Lu-DOTA-DN(PTX)-BN for Selective and Concomitant Radio and Drug—Therapeutic E ect on Breast Cancer Cells es
dc.type Artículo es
dc.provenance Científica es
dc.road Verde es
dc.organismo Química es
dc.ambito Nacional es
dc.cve.CenCos 20401 es
dc.cve.progEstudios 724 es
dc.audience students es
dc.audience researchers es
dc.type.conacyt article
dc.identificator 2
dc.relation.doi 10.3390/polym11101572


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  • Título
  • Synthesis and Evaluation of 177Lu-DOTA-DN(PTX)-BN for Selective and Concomitant Radio and Drug—Therapeutic E ect on Breast Cancer Cells
  • Autor
  • GIBBENS BANDALA, BRENDA VIANEY
  • MORALES AVILA, ENRIQUE
  • FERRO FLORES, GUILLERMINA
  • SANTOS CUEVAS, CLARA LETICIA
  • LUNA GUTIERREZ, MYRNA ALEJANDRA
  • RAMIREZ NAVA, GERARDO JULIAN
  • OCAMPO GARCIA, BLANCA ELI
  • Fecha de publicación
  • 2019-09-27
  • Editor
  • Polymers, MDPI
  • Tipo de documento
  • Artículo
  • Palabras clave
  • polymeric nanosystems
  • dendrimers
  • radiotherapy
  • GRPr
  • paclitaxel
  • lutetium-177
  • Los documentos depositados en el Repositorio Institucional de la Universidad Autónoma del Estado de México se encuentran a disposición en Acceso Abierto bajo la licencia Creative Commons: Atribución-NoComercial-SinDerivar 4.0 Internacional (CC BY-NC-ND 4.0)

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