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Efficacy, biodistribution, and nephrotoxicity of experimental amphotericin B-deoxycholate formulations for pulmonary aspergillosis

  • Alicia López-Sánchez
  • , Alba Pérez-Cantero
  • , Carlos Torrado-Salmerón
  • , Adela Martin-Vicente
  • , Víctor García-Herrero
  • , María Ángeles González-Nicolás
  • , Alberto Lázaro
  • , Alberto Tejedor
  • , Santiago Torrado-Santiago
  • , Juan José García-Rodríguez
  • , Javier Capilla
  • , Susana Torradoa*
  • *Autor correspondiente de este trabajo

Producción científica: Contribución a una revistaArtículorevisión exhaustiva

10 Citas (Scopus)

Resumen

An experimental micellar formulation of 1:1.5 amphotericin B-sodium deoxycholate (AMB:DCH 1:1.5) was obtained and characterized to determine its aggregation state and particle size. The biodistribution, nephrotoxicity, and efficacy against pulmonary aspergillosis in a murine model were studied and compared to the liposomal commercial formulation of amphotericin B after intravenous administration. The administration of 5 mg/kg AMB:DCH 1:1.5 presented 2.8-fold-higher lung concentrations (18.125 3.985 g/g after 6 daily doses) and lower kidney exposure (0.391 0.167 g/g) than liposomal commercial amphotericin B (6.567 1.536 and 5.374 1.157 g/g in lungs and kidneys, respectively). The different biodistribution of AMB:DCH micelle systems compared to liposomal commercial amphotericin B was attributed to their different morphologies and particle sizes. The efficacy study has shown that both drugs administered at 5 mg/kg produced similar survival percentages and reductions of fungal burden. A slightly lower nephrotoxicity, associated with amphotericin B, was observed with AMB:DCH 1:1.5 than the one induced by the liposomal commercial formulation. However, AMB:DCH 1:1.5 reached higher AMB concentrations in lungs, which could represent a therapeutic advantage over liposomal commercial amphotericin B-based treatment of pulmonary aspergillosis. These results are encouraging to explore the usefulness of AMB:DCH 1:1.5 against this disease.

Idioma originalInglés
Número de artículoe00489-18
PublicaciónAntimicrobial Agents and Chemotherapy
Volumen62
N.º7
DOI
EstadoPublicada - jul 2018
Publicado de forma externa

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