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1.
001-es BibID:
BIBFORM125597
035-os BibID:
(scopus)85207761844 (wos)001348191500001
Első szerző:
Benziane, Anass (molekuláris biológus)
Cím:
Synergistic effect of folic acid and hypericin administration to improve the efficacy of photodynamic therapy via folate receptors / Benziane Anass, Huntosová Veronika, Pevná Viktória, Zauska Lubos, Vámosi György, Hovan Andrej, Zelenková Gabriela, Zelenák Vladimír, Almási Miroslav
Dátum:
2024
ISSN:
1011-1344 1873-2682
Megjegyzések:
Transport systems are developed to improve the solubility of the transported drug, increase its stability, enhance its pharmacological activity and target cancer while minimising side effects. In this work, nanoporous silica particles that can be functionalized and loaded with a large number of hydrophobic molecules are proposed. The designed system was modified with folic acid to target the folic acid receptors of cancer cells. This modification enabled a higher uptake of the drug by the cells. Hypericin was selected as a hydrophobic molecule/drug with photodynamic properties suitable for diagnosis and therapy. Fluorescence microscopy and flow cytometry were used to detect the targeting and distribution of hypericin in the cancer cells. Furthermore, the combination of folic acid and hypericin has been shown to form singlet oxygen and to have a synergistic effect in improving the efficacy of photodynamic therapy. The functionalisation of the particles proposed in this work holds great potential for the delivery of hydrophobic drugs to other types of cancer cells with increased expression of the folic acid receptor to which the particles can be attached.
Tárgyszavak:
Orvostudományok
Elméleti orvostudományok
idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
Mesoporous silica
SBA-15
Folate receptors
Targeting
Hypericin
Photodynamic therapy
Transport
Megjelenés:
Journal Of Photochemistry And Photobiology B-Biology. - 261 (2024), p. 1-14. -
További szerzők:
Huntošová, Veronika
Pevná, Viktória
Zauška, Ľuboš
Vámosi György (1967-) (biofizikus)
Hovan, Andrej
Zelenková, Gabriela
Zeleňák, Vladimír
Almáši, Miroslav
Internet cím:
Szerző által megadott URL
DOI
Intézményi repozitóriumban (DEA) tárolt változat
Borító:
Saját polcon:
2.
001-es BibID:
BIBFORM116504
035-os BibID:
(scopus)85170688343 (wos)001081473700001
Első szerző:
Pevná, Viktória
Cím:
Effective transport of aggregated hypericin encapsulated in SBA-15 nanoporous silica particles for photodynamic therapy of cancer cells / Pevná Viktória, Zauska Lubos, Benziane Anass, Vámosi György, Girman Vladimír, Miklósová Monika, Zelenák Vladimír, Huntosová Veronika, Almási Miroslav
Dátum:
2023
ISSN:
1011-1344 1873-2682
Megjegyzések:
Photodynamic therapy (PDT) represents an interesting modality for the elimination of damaged biomaterials and cells. This treatment takes advantage of the photosensitizing properties of molecules that are active only when irradiated with light. In the present work, a dual property of hypericin, a hydrophobic molecule with high performance in photodiagnostics and photodynamic therapy, was exploited. The non-fluorescent and photodynamically inactive form of hypericin aggregates was loaded into the nanopores of SBA-15 silica particles. The synthesized particles were characterized by infrared spectroscopy, thermogravimetry, differential thermal analysis, small-angle X-ray scattering and transmission electron microscopy. Hypericin aggregates were confirmed by absorption spectra typical of aggregated hypericin and by its short fluorescence lifetime. Release of hypericin from the particles was observed toward serum proteins, mimicking physiological conditions. Temperature- and time-dependent uptake of hypericin by cancer cells showed gradual release of hypericin from the particles and active cellular transport by endocytosis. A closer examination of SBA-15-hypericin uptake by fluorescence lifetime imaging showed that aggregated hypericin molecules, characterized by a short fluorescence lifetime (?4 ns), were still present in the SBA-15 particles upon uptake by cells. However, monomerization of hypericin in cancer cells was observed by extending the hypericin fluorescence lifetime by ?8 ns, preferentially in lipid compartments and the plasma membrane. This suggests a promising prognosis for delayed biological activity of the entire cargo, which was confirmed by effective PDT in vitro. In summary, this work presents an approach for safe, inactive delivery of hypericin that is activated at the target site in cells and tissues.
Tárgyszavak:
Orvostudományok
Klinikai orvostudományok
idegen nyelvű folyóiratközlemény külföldi lapban
folyóiratcikk
Nanoporous silica
Hypericin
Transport
Cancer cells
Fluorescence lifetime
Photodynamic therapy
Megjelenés:
Journal Of Photochemistry And Photobiology B-Biology. - 247 (2023), p. 1-11. -
További szerzők:
Zauška, Ľuboš
Benziane, Anass (1990-) (molekuláris biológus)
Vámosi György (1967-) (biofizikus)
Girman, Vladimír
Miklóšová, Monika
Zeleňák, Vladimír
Huntošová, Veronika
Almáši, Miroslav
Internet cím:
Szerző által megadott URL
DOI
Intézményi repozitóriumban (DEA) tárolt változat
Borító:
Saját polcon:
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