Rational Design, Synthesis and Evaluation of CD-Containing as a Prednisone Delivery Platform
Fecha
2018Autor
Marican, Adolfo [Chile. Universidad de Talca]
Valdéz, Oscar [Chile. Universidad Católica del Maule]
Wehinger, Sergio [Chile. Universidad de Talca]
Villaseñor, Jorge [Chile. Universidad de Talca]
Fuentealba, Natalia [Chile. Universidad de Talca]
Arenas-Salinas, Mauricio [Chile. Universidad de Talca]
Argandoña, Yerko [Chile. Universidad de Talca]
Carrasco-Sánchez, Verónica [Chile. Universidad de Talca]
Durán-Lara, Estebán F. [Chile. Universidad de Talca]
Avila-Salas, F. [Chile. Universidad Mayor. Facultad de Ciencias. Centro de Nanotecnología Aplicada]
Ubicación geográfica
Notas
HERRAMIENTAS
Resumen
This study describes the in-silico rational design, synthesis and evaluation of cross-linked polyvinyl alcohol hydrogels containing γ-cyclodextrin (γ-CDHSAs) as platforms for the sustained release of prednisone (PDN). Through in-silico studies using semi-empirical quantum mechanical calculations, the effectiveness of 20 dicarboxylic acids to generate a specific cross-linked hydrogel capable of supporting different amounts of γ-cyclodextrin (γ-CD) was evaluated. According to the interaction energies calculated with the in-silico studies, the hydrogel made from PVA cross-linked with succinic acids (SA) was shown to be the best candidate for containing γ-CD. Later, molecular dynamics simulation studies were performed in order to evaluate the intermolecular interactions between PDN and three cross-linked hydrogel formulations with different proportions of γ-CD (2.44%, 4.76% and 9.1%). These three cross-linked hydrogels were synthesized and characterized. The loading and the subsequent release of PDN from the hydrogels were investigated. The in-silico and experimental results showed that the interaction between PDN and γ-CDHSA was mainly produced with the γ-CDs linked to the hydrogels. Thus, the unique structures and properties of γ-CDHSA demonstrated an interesting multiphasic profile that could be utilized as a promising drug carrier for controlled, sustained and localized release of PDN.
URI
http://repositorio.umayor.cl/xmlui/handle/sibum/2483http://www.mdpi.com/1999-4923/10/1/30
https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5874843/pdf/pharmaceutics-10-00030.pdf
https://doi.org/10.3390/pharmaceutics10010030
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