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dc.contributor.author Ancira Cortez, Alejandra
dc.contributor.author Ferro Flores, Guillermina
dc.contributor.author Jimenez Mancilla, Nallely Patricia
dc.contributor.author Morales Avila, Enrique
dc.contributor.author Trujillo Benitez, Diana Sarahí
dc.contributor.author Ocampo García, Blanca Eli
dc.contributor.author Santos Cuevas, Clara Leticia
dc.contributor.author Escudero Castellanos, Alondra
dc.contributor.author Luna Gutierrez, Myrna
dc.date.accessioned 2021-02-11T02:14:41Z
dc.date.available 2021-02-11T02:14:41Z
dc.date.issued 2020-08-07
dc.identifier.issn 0928-4931
dc.identifier.uri http://hdl.handle.net/20.500.11799/109877
dc.description.abstract Among the nanomaterials, rare sesquioxides (lanthanide oxides such as Lu2O3) are of interest due to their adequate thermal conductivity, excellent chemical stability, and high light output. The prostate-specific membrane antigen (PSMA) is an integral multifunctional protein overexpressed in various types of cancer cells. The radiolabeled PSMA inhibitor peptides (iPSMA) have demonstrated their usefulness as specific probes in the treatment and detection of a wide variety of neoplasms, mainly due to their high in vivo recognition by the PSMA protein. The objective of this research was to synthesize Lu2O3-iPSMA nanoparticles (NPs) and characterize their physicochemical properties before and after neutron activation, as well as to assess their biodistribution profile and in vitro potential to target cells overexpressing PSMA. The Lu2O3 NPs were synthesized by the precipitationcalcination method and conjugated to the iPSMA peptide using DOTA (1,4,7,10-tetraazocyclodecane-N,N′,N″,N‴-tetraacetic acid) as a linking agent. Results of the physicochemical characterization by FT-IR and UV–Vis spectroscopies, SEM, TEM, DLS, HRTEM, SAED, DSC-TGA, and X-ray diffraction indicated the formation of Lu2O3-iPSMA NPs (diameter of 29.98 ± 9.07 nm), which were not affected in their physicochemical properties after neutron activation. 177Lu2O3-iPSMA NPs showed high affinity (Kd = 5.7 ± 1.9 nM) for the PSMA protein, evaluated by the saturation assay on HepG2 hepatocellular carcinoma cells (PSMA-positive). The biodistribution profile of the nanosystem in healthy mice showed the main uptake in the liver. After irradiation, radioactive Lu2O3-iPSMA NPs exhibited radioluminescent properties, making the in vivo acquisition of their biodistribution, via optical imaging, possible. The results obtained from this research validate the execution of additional preclinical studies with the objective of evaluating the potential of the 177Lu2O3-iPSMA NPs for the targeted radiotherapy and in vivo imaging of tumors overexpressing the PSMA protein. es
dc.description.sponsorship Mexican National Council of Science and Technology (CONACyT) grant CB2017-2018-A1-S-36841 es
dc.language.iso eng es
dc.publisher Materials Science & Engineering C es
dc.rights embargoedAccess es
dc.rights.uri http://creativecommons.org/licenses/by/4.0 es
dc.subject Lu2O3 nanoparticles es
dc.subject iPSMA peptide es
dc.subject 177Lu2O3-iPSMA nanoparticles es
dc.subject Radioluminescence es
dc.subject Targeted radiotherapy es
dc.subject.classification BIOLOGÍA Y QUÍMICA es
dc.title Synthesis, chemical and biochemical characterization of Lu2O3-iPSMA nanoparticles activated by neutron irradiation es
dc.type Apuntes es
dc.provenance Científica es
dc.road Dorada es
dc.organismo Química es
dc.ambito Internacional es
dc.cve.CenCos 20401 es
dc.relation.vol 117


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  • Título
  • Synthesis, chemical and biochemical characterization of Lu2O3-iPSMA nanoparticles activated by neutron irradiation
  • Autor
  • Ancira Cortez, Alejandra
  • Ferro Flores, Guillermina
  • Jimenez Mancilla, Nallely Patricia
  • Morales Avila, Enrique
  • Trujillo Benitez, Diana Sarahí
  • Ocampo García, Blanca Eli
  • Santos Cuevas, Clara Leticia
  • Escudero Castellanos, Alondra
  • Luna Gutierrez, Myrna
  • Fecha de publicación
  • 2020-08-07
  • Editor
  • Materials Science & Engineering C
  • Tipo de documento
  • Apuntes
  • Palabras clave
  • Lu2O3 nanoparticles
  • iPSMA peptide
  • 177Lu2O3-iPSMA nanoparticles
  • Radioluminescence
  • Targeted radiotherapy
  • 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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