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Título
A Micellar Formulation of Quercetin Prevents Cisplatin Nephrotoxicity
Autor(es)
Palabras clave
cisplatin; nephrotoxicity; flavonoid; quercetin; nephroprotection; bioavailability; kidney; micelles; solubility; formulation
Fecha de publicación
2021
Editor
MDPI
Citación
Casanova AG, Prieto M, Colino CI, Gutiérrez-Millán C, Ruszkowska-Ciastek B, de Paz E, Martín Á, Morales AI, López-Hernández FJ. A Micellar Formulation of Quercetin Prevents Cisplatin Nephrotoxicity. Int J Mol Sci. 2021 Jan 13;22(2):729. doi: 10.3390/ijms22020729. PMID: 33450917; PMCID: PMC7828436.
Resumen
The antioxidant flavonoid quercetin has been shown to prevent nephrotoxicity in animal
models and in a clinical study and is thus a very promising prophylactic candidate under development.
Quercetin solubility is very low, which handicaps clinical application. The aim of this work
was to study, in rats, the bioavailability and nephroprotective efficacy of a micellar formulation of
Pluronic F127-encapsulated quercetin (P-quercetin), with improved hydrosolubility. Intraperitoneal
administration of P-quercetin leads to an increased plasma concentration and bioavailability of
quercetin compared to the equimolar administration of natural quercetin. Moreover, P-quercetin
retains overall nephroprotective properties, and even slightly improves some renal function parameters,
when compared to natural quercetin. Specifically, P-quercetin reduced the increment in plasma
creatinine (from 3.4 0.5 to 1.2 0.3 mg/dL) and urea (from 490.9 43.8 to 184.1 50.1 mg/dL) and
the decrease in creatinine clearance (from 0.08 0.02 to 0.58 0.19 mL/min) induced by the nephrotoxic
chemotherapeutic drug cisplatin, and it ameliorated histological evidence of tubular damage.
This new formulation with enhanced kinetic and biopharmaceutical properties will allow for further
exploration of quercetin as a candidate nephroprotector at lower dosages and by administration
routes oriented towards its clinical use.
URI
ISSN
1422-0067
DOI
10.3390/ijms22020729
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