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dc.contributor.author GALLAGA GONZALEZ, JAIME
dc.contributor.author MORALES AVILA, ENRIQUE
dc.contributor.author TORRES GARCIA, EUGENIO
dc.contributor.author Estrada Godínez, José Antonio
dc.contributor.author DIAZ SANCHEZ, LUIS ENRIQUE
dc.contributor.author IZQUIERDO SAEZ, GERMAN
dc.contributor.author ARANDA LARA, LILIANA
dc.contributor.author ISAAC OLIVE, KEILA
dc.creator GALLAGA GONZALEZ, JAIME; 664788
dc.creator MORALES AVILA, ENRIQUE; 170668
dc.creator TORRES GARCIA, EUGENIO; 49824
dc.creator Estrada Godínez, José Antonio; 41791
dc.creator DIAZ SANCHEZ, LUIS ENRIQUE; 103051
dc.creator IZQUIERDO SAEZ, GERMAN; 367408
dc.creator ARANDA LARA, LILIANA; 473137
dc.creator ISAAC OLIVE, KEILA; 243975
dc.date.accessioned 2023-02-11T00:05:16Z
dc.date.available 2023-02-11T00:05:16Z
dc.date.issued 2022-06-30
dc.identifier.uri http://hdl.handle.net/20.500.11799/137811
dc.description.abstract Cerenkov radiation (CR) can be used as an internal light source in photodynamic therapy (PDT). Methotrexate (MTX) and paclitaxel (PTX), chemotherapeutic agents with wide clinical use, have characteristics of photosensitizers (PS). This work evaluates the possibility of photoexciting MTX and PTX with CR from 18F-FDG to produce reactive oxygen species (ROS) capable of inducing cytotoxicity. PTX did not produce ROS when excited by CR from 18F-FDG, so it is not useful for PDT. In contrast, MTX produces 1O2 (detected by ABMA) in amounts sufficient to significantly decrease the viability of the T47D cells. MTX solutions of 100 nM combined with 18F-FDG activities of 50 (1.85 MBq) and 100 μCi (3.7 MBq) produced a significant decrease in cell viability to (50.09 ± 4.95) and (47.96 ± 11.19)%, respectively, compared to MTX (66.29 ± 5.92)% and 18F-FDG (91.35 ± 7.00% for 50 μCi and 99.43 ± 11.03% for 100 μCi) alone. Using the CellRox Green reagent, the intracellular production of ROS was confirmed as the main mechanism of cytotoxicity. The results confirm the therapeutic potential of photoactivation with CR and the synergy of the combined treatment with chemotherapy + photodynamic therapy (CMT + PDT). The combination of chemotherapeutic agents with PS properties and β-emitting radiopharmaceuticals, previously approved for clinical use, will make it possible to shorten the evaluation stages of new CMT + PDT systems. es
dc.description.sponsorship CONACyT: 2021-316833 COMECyT: FICDTEM-2021-015 es
dc.language.iso eng es
dc.publisher ACS publications es
dc.rights openAccess es
dc.rights.uri http://creativecommons.org/licenses/by-nc-nd/4.0
dc.subject Photoactivation es
dc.subject Cerenkov es
dc.subject Chemo-Photodynamic Therapy es
dc.subject Radiotherapy es
dc.subject.classification BIOLOGÍA Y QUÍMICA
dc.title Photoactivation of Chemotherapeutic Agents with Cerenkov Radiation for Chemo-Photodynamic Therapy es
dc.type Artículo es
dc.provenance Científica es
dc.road Verde es
dc.organismo Medicina es
dc.ambito Internacional es
dc.cve.CenCos 20201 es
dc.cve.progEstudios 6129 es
dc.audience students es
dc.audience researchers es
dc.type.conacyt article
dc.identificator 2
dc.relation.vol 7


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  • Título
  • Photoactivation of Chemotherapeutic Agents with Cerenkov Radiation for Chemo-Photodynamic Therapy
  • Autor
  • GALLAGA GONZALEZ, JAIME
  • MORALES AVILA, ENRIQUE
  • TORRES GARCIA, EUGENIO
  • Estrada Godínez, José Antonio
  • DIAZ SANCHEZ, LUIS ENRIQUE
  • IZQUIERDO SAEZ, GERMAN
  • ARANDA LARA, LILIANA
  • ISAAC OLIVE, KEILA
  • Fecha de publicación
  • 2022-06-30
  • Editor
  • ACS publications
  • Tipo de documento
  • Artículo
  • Palabras clave
  • Photoactivation
  • Cerenkov
  • Chemo-Photodynamic Therapy
  • 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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