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Solubility Determination of c-Met Inhibitor in Solvent Mixtures and Mathematical Modeling to Develop Nanosuspension Formulationopen access

Authors
Ravi, MaharjanJulu, TripathiKim, Nam AhPark, Kyeung EuiJeong, Seong Hoon
Issue Date
Jan-2021
Publisher
MDPI
Keywords
transcutol(&#174); HP; thermodynamics; solubility; nanosuspension; mathematical models; precipitation
Citation
MOLECULES, v.26, no.2
Indexed
SCIE
SCOPUS
Journal Title
MOLECULES
Volume
26
Number
2
URI
https://scholarworks.dongguk.edu/handle/sw.dongguk/19445
DOI
10.3390/molecules26020390
ISSN
1420-3049
1420-3049
Abstract
The solubility and dissolution thermodynamics of new c-Met inhibitor, ABN401, were determined in eleven solvents and Transcutol(R) HP-water mixture (TWM) from 298.15 to 318.15 K. The experimental solubilities were validated using five mathematical models, namely modified Apelblat, van't Hoff, Buchowski-Ksiazaczak lambda h, Yalkowsky, and Jouyban-Acree van't Hoff models. The experimental results were correlated and utilized further to investigate the feasibility of nanosuspension formation using liquid anti-solvent precipitation. Thermodynamic solubility of ABN401 increased significantly with the increase in temperature and maximum solubility was obtained with Transcutol(R) HP while low solubility in was obtained water. An activity coefficient study indicated that high molecular interaction was observed in ABN401-Transcutol(R) HP (THP). The solubility increased proportionately as the mole fraction of Transcutol(R) HP increased in TWM, which was also supported by a solvent effect study. The result suggested endothermic and entropy-driven dissolution. Based on the solubility, nanosuspension was designed with Transcutol(R) HP as solvent, and water as anti-solvent. The mean particle size of nanosuspension decreased to 43.05 nm when the mole fraction of ABN401 in THP, and mole fraction of ABN401 in TWM mixture were decreased to 0.04 and 0.1. The ultrasonicated nanosuspension appeared to give comparatively higher dissolution than micronized nanosuspension and provide a candidate formulation for in vivo purposes.
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