Improving and measuring the solubility of favipiravir and montelukast in SC-CO2 with ethanol projecting their nanonization
Abstract
Supercritical carbon dioxide (SC-CO2)-based approaches have become more popular in recent years as alternative methods for creating micro- or nanosized medicines. Particularly, high drug solubility is required in those techniques using SC-CO2 as a solvent. During the most recent pandemic years, favipiravir and montelukast were two of the most often prescribed medications for the treatment of COVID-19. In this study, ethanol at 1 and 3 mol% was utilized as a cosolvent to increase the solubility of both medicines in SC-CO2 by a static approach using a range of temperatures (308 to 338 K) and pressure (12 to 30 MPa) values. The experimentally determined solubilities of favipiravir and montelukast in SC-CO2 + 3 mol% ethanol showed solubility values up to 33.3 and 24.5 times higher than that obtained for these drugs with only SC-CO2. The highest values were achieved in the pressure of 12 MPa and temperature of 338 K. Last but not least, six density-based semi-empirical models with various adjustable parameters were used to perform the modeling of the solubility of favipiravir and montelukast.
Más información
Título según SCOPUS: | ID SCOPUS_ID:85178066798 Not found in local SCOPUS DB |
Título de la Revista: | RSC ADVANCES |
Volumen: | 13 |
Editorial: | ROYAL SOC CHEMISTRY |
Fecha de publicación: | 2023 |
Página de inicio: | 34210 |
Página final: | 34223 |
DOI: |
10.1039/D3RA05484E |
Notas: | SCOPUS |