Development and in vitro evaluation of solid dispersions as strategy to improve albendazole biopharmaceutical behavior

Simonazzi, Analía; Cid, Alicia Graciela; Paredes, Alejandro Javier; Schofs, Laureano; Gonzo, Elio Emilio; Palma, Santiago Daniel; Bermudez, Jose Maria

info:eu-repo/semantics/article

Fecha

2018-09

Registro en:

Simonazzi, Analía; Cid, Alicia Graciela; Paredes, Alejandro Javier; Schofs, Laureano; Gonzo, Elio Emilio; et al.; Development and in vitro evaluation of solid dispersions as strategy to improve albendazole biopharmaceutical behavior; Future Medicine Ltd.; Therapeutic Delivery; 9; 9; 9-2018; 623-638

2041-5990

http://hdl.handle.net/11336/92358

2041-6008

CONICET Digital

CONICET

https://repositorioslatinoamericanos.uchile.cl/handle/2250/4376716

Autor

Simonazzi, Analía

Cid, Alicia Graciela

Paredes, Alejandro Javier

Schofs, Laureano

Gonzo, Elio Emilio

Palma, Santiago Daniel

Bermudez, Jose Maria

Institución

Consejo Nacional de Investigaciones Científicas y Tecnológicas (Argentina)

Resumen

Solid dispersions using Poloxamer 407 as carrier were developed to improvealbendazole (ABZ) solubility and dissolution profiles. ABZ/poloxamer solid dispersions were prepared, and dissolution profiles were mathematically modeled and compared with physical mixtures, pharmaceutical ABZ and a commercial formulation. Results: Poloxamer 407 increased exponentially ABZ solubility, in about 400% when 95% w/w of polymer compared with its absence. Solid dispersions initial dissolution rate was three to 20-fold higher than physical mixtures, the drug and the commercial formulation. All the solid dispersions required less than 2.2 min to reach an 80% of ABZ dissolution, while the commercial formulation needed around 40 min. Conclusion: Solid dispersions improved ABZ solubility and dissolution rate, which could result in a faster absorption and an increased bioavailability.

Materias

ALBENDAZOLE

DISSOLUTION EFFICIENCY

INITIAL DISSOLUTION RATE

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