Your search keyword '"Bermejo, Marival"' showing total 7 results

1. In silico, in situ, in vitro, and in vivo predictive methods for modeling formulation performance

Author

Bermejo, Marival, primary, Camara-Martinez, Irene, additional, Sanchez-Dengra, Barbará, additional, Ruiz-Picazo, Alejandro, additional, Gonzalez-Alvarez, Isabel, additional, and Gonzalez-Alvarez, Marta, additional

Published

2024

2. Pharmaceutical Compounding in Veterinary Medicine: Suspension of Itraconazole

Author

Generalitat Valenciana, Agencia Estatal de Investigación, European Regional Development Fund, Cabañero-Resta, Gema J., Sánchez-Dengra, Bárbara, Ruiz Picazo, Alejandro, Bermejo, Marival, Merino Sanjuan, Virginia, González-Álvarez, Isabel, González-Álvarez, Marta, Generalitat Valenciana, Agencia Estatal de Investigación, European Regional Development Fund, Cabañero-Resta, Gema J., Sánchez-Dengra, Bárbara, Ruiz Picazo, Alejandro, Bermejo, Marival, Merino Sanjuan, Virginia, González-Álvarez, Isabel, and González-Álvarez, Marta

Abstract

[EN] Itraconazole is a drug used in veterinary medicine for the treatment of different varieties of dermatophytosis at doses between 3-5 mg/kg/day in cats. Nevertheless, in Spain, it is only available in the market as a 52 mL suspension at 10 mg/mL. The lack of alternative formulations, which provide sufficient formulation to cover the treatment of large animals or allow the treatment of a group of them, can be overcome with compounding. For this purpose, it has to be considered that itraconazole is a weak base, class II compound, according to the Biopharmaceutics Classification System, that can precipitate when reaching the duodenum. The aim of this work is to develop alternative oral formulations of itraconazole for the treatment of dermatophytosis. Several oral compounds of itraconazole were prepared and compared, in terms of dissolution rate, permeability, and stability, in order to provide alternatives to the medicine commercialized. The most promising formulation contained hydroxypropyl methylcellulose and beta-cyclodextrin. This combination of excipients was capable of dissolving the same concentration as the reference product and delaying the precipitation of itraconazole upon leaving the stomach. Moreover, the intestinal permeability of itraconazole was increased more than two-fold.

Published

2024

3. In Vivo Predictive Dissolution and Biopharmaceutic-Based In Silico Model to Explain Bioequivalence Results of Valsartan, a Biopharmaceutics Classification System Class IV Drug

Author

Gonzalez-Alvarez, Isabel, primary, Ruiz-Picazo, Alejandro, additional, Selles-Talavera, Ruben, additional, Figueroa-Campos, Andres, additional, Merino, Virginia, additional, Bermejo, Marival, additional, and Gonzalez-Alvarez, Marta, additional

Published

2024

4. Alternative methodology for the study of brain distribution of drugs with in vitro tests.

Author

Sanchez-Dengra, Barbara, primary, Gonzalez-Alvarez, Isabel, additional, Gonzalez-Alvarez, Marta, additional, and Bermejo, Marival, additional

Published

2024

5. Pharmaceutical Compounding in Veterinary Medicine: Suspension of Itraconazole.

Author

Cabañero-Resta, Gema J., Sánchez-Dengra, Bárbara, Ruiz-Picazo, Alejandro, Bermejo, Marival, Merino, Virginia, Gonzalez-Alvarez, Isabel, and Gonzalez-Alvarez, Marta

Subjects

ITRACONAZOLE, VETERINARY medicine, INTESTINAL barrier function, ANIMAL welfare, VETERINARY drugs, CYCLODEXTRINS

Abstract

Itraconazole is a drug used in veterinary medicine for the treatment of different varieties of dermatophytosis at doses between 3–5 mg/kg/day in cats. Nevertheless, in Spain, it is only available in the market as a 52 mL suspension at 10 mg/mL. The lack of alternative formulations, which provide sufficient formulation to cover the treatment of large animals or allow the treatment of a group of them, can be overcome with compounding. For this purpose, it has to be considered that itraconazole is a weak base, class II compound, according to the Biopharmaceutics Classification System, that can precipitate when reaching the duodenum. The aim of this work is to develop alternative oral formulations of itraconazole for the treatment of dermatophytosis. Several oral compounds of itraconazole were prepared and compared, in terms of dissolution rate, permeability, and stability, in order to provide alternatives to the medicine commercialized. The most promising formulation contained hydroxypropyl methylcellulose and β-cyclodextrin. This combination of excipients was capable of dissolving the same concentration as the reference product and delaying the precipitation of itraconazole upon leaving the stomach. Moreover, the intestinal permeability of itraconazole was increased more than two-fold. [ABSTRACT FROM AUTHOR]

Published

2024

6. Intestinal Permeability of β-Lapachone and Its Cyclodextrin Complexes and Physical Mixtures

Author

Mangas-Sanjuan, Victor, Gutiérrez-Nieto, Jorge, Echezarreta-López, Magdalena, González-Álvarez, Isabel, González-Álvarez, Marta, Casabó, Vicente-Germán, Bermejo, Marival, and Landin, Mariana

Abstract

β-Lapachone (βLAP) is a promising, poorly soluble, antitumoral drug. βLAP combination with cyclodextrins (CDs) improves its solubility and dissolution but there is not enough information about the impact of cyclodextrins on βLAP intestinal permeability. The objectives of this work were to characterize βLAP intestinal permeability and to elucidate cyclodextrins effect on the dissolution properties and on the intestinal permeability. The final goal was to evaluate CDs influence on the oral absorption of βLAP. Binary systems (physical mixtures and inclusion complexes) including βLAP and CDs (β-cyclodextrin: βCD, random-methyl-β-cyclodextrin: RMβCD and sulfobutylether-β-cyclodextrin: SBEβCD) have been prepared and analysed by differential scanning calorimetry. βLAP (and its combinations with CDs) absorption rate coefficients and effective permeability values have been determined in vitro in MDCK or MDCK-Mdr1 monolayers and in situ in rat by a closed loop perfusion technique. DSC results confirmed the formation of the inclusion complexes. βLAP–CDs inclusion complexes improve drug solubility and dissolution rate in comparison with physical mixtures. βLAP presented a high permeability value which can provide complete oral absorption. Its oral absorption is limited by its low solubility and dissolution rate. Cyclodextrin (both as physical mixtures and inclusion complexes) showed a positive effect on the intestinal permeability of βLAP. Complexation with CDs does not reduce βLAP intestinal permeability in spite of the potential negative effect of the reduction in free fraction of the drug. The use of RMβCD or SBEβCD inclusion complexes could benefit βLAP oral absorption by enhancing its solubility, dissolution rate and permeability.

Published

2024

7. Ionic Hydrogel Based on Chitosan Cross-Linked with 6-Phosphogluconic Trisodium Salt as a Drug Delivery System

Author

Martínez-Martínez, Mayte, Rodríguez-Berna, Guillermo, Gonzalez-Alvarez, Isabel, Hernández, MaJesús, Corma, Avelino, Bermejo, Marival, Merino, Virginia, and Gonzalez-Alvarez, Marta

Abstract

In this work, 6-phosphogluconic trisodium salt (6-PG–Na+) is introduced as a new aqueous and nontoxic cross-linking agent to obtain ionic hydrogels. Here, it is shown the formation of hydrogels based on chitosan cross-linked with 6-PG–Na+. This formulation is obtained by ionic interaction of cationic groups of polymer with anionic groups of the cross-linker. These hydrogels are nontoxic, do not cause dermal irritation, are easy to extend, and have an adequate adhesion force to be applied as polymeric film over the skin. This formulation exhibits a first order release kinetic and can be applied as drug vehicle for topical administration or as wound dressing for wound healing. The primary goal of this communication is to report the identification and utility of 6-phosphogluconic trisodium salt (6-PG–Na+) as a nontoxic cross-linker applicable for cationic polymers.

Published

2024