High energy ball milling vs. nano spray drying in the development of supersaturated systems loaded with bosentan

[Display omitted] In this study, high energy ball milling and nano spray drying were used to prepare amorphous solid dispersions of bosentan in copovidone for the first time. In particular, the impact of this polymer on the bosentan amorphization kinetics was investigated. Copovidone was shown to fa...

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Published in:European journal of pharmaceutics and biopharmaceutics 2023-07, Vol.188, p.137-146
Main Authors: Krupa, Anna, Danède, Florence, Majda, Dorota, Węgrzyn, Agnieszka, Strojewski, Dominik, Kondera, Ita, Willart, Jean-François
Format: Article
Language:English
Subjects:
Bosentan
Condensed Matter
Disordered Systems and Neural Networks
Drug Compounding - methods
Enabling formulations
Materials Science
Mechanical activation
Physics
Poorly soluble drugs
Pyrrolidines - chemistry
Soft Condensed Matter
Solubility
Solvent evaporation
Supersaturation
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Summary:[Display omitted] In this study, high energy ball milling and nano spray drying were used to prepare amorphous solid dispersions of bosentan in copovidone for the first time. In particular, the impact of this polymer on the bosentan amorphization kinetics was investigated. Copovidone was shown to facilitate the amorphization of bosentan upon ball milling. As a result, bosentan was dispersed in copovidone at the molecular level, forming amorphous solid dispersions, regardless of the ratio of the compounds. The similarity between the values of the adjustment parameter that describes the goodness of fit of the Gordon-Taylor equation to the experimental data (K = 1.16) and that theoretically calculated for an ideal mixture (K = 1.13) supported these findings. The kind of coprocessing method determined the powder microstructure and the release rate. The opportunity to prepare submicrometer-sized spherical particles using nano spray drying was an important advantage of this technology. Both coprocessing methods allowed the formation of long-lasting supersaturated bosentan solutions in the gastric environment with maximum concentrations reached ranging from four (11.20 μg/mL) to more than ten times higher (31.17 μg/mL) than those recorded when the drug was vitrified alone (2.76 μg/mL). Moreover, this supersaturation lasted for a period of time at least twice as long as that of the amorphous bosentan processed without copovidone (15 min vs. 30–60 min). Finally, these binary amorphous solid dispersions were XRD-amorphous for a year of storage under ambient conditions.
ISSN:0939-6411
1873-3441
DOI:10.1016/j.ejpb.2023.05.014