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Captopril oral solution for pediatric use: formulation, stability study and palatability assessment in vivo
Dysarz, Leticia Pereira; Tavares, Melanie; Viçosa, Alessandra Lifsitch; Ribeiro, Mara Fernandes; Teixeira, Rafaela Gomes de Silva; Elias, Sabrina Calil; Silva, Márcio Robert Mattos da; Santos, Elisabete Pereira dos; Ricci-Júnior, Eduardo.
Affiliation
  • Dysarz, Leticia Pereira; Federal University of Rio de Janeiro. Faculty of Pharmacy. Laboratório de Desenvolvimento Galênico. Rio de Janeiro. BR
  • Tavares, Melanie; Federal University of Rio de Janeiro. Faculty of Pharmacy. Laboratório de Desenvolvimento Galênico. Rio de Janeiro. BR
  • Viçosa, Alessandra Lifsitch; Fiocruz. Institute of Technology in Drugs, Farmanguinhos. Laboratório de Farmacotécnica Experimental. Rio de Janeiro. BR
  • Ribeiro, Mara Fernandes; Fluminense Federal University. Faculty of Pharmacy. Laboratório de Farmacologia. Niterói. BR
  • Teixeira, Rafaela Gomes de Silva; Fluminense Federal University. Faculty of Pharmacy. Laboratório de Farmacologia. Niterói. BR
  • Elias, Sabrina Calil; Fluminense Federal University. Faculty of Pharmacy. Laboratório de Farmacologia. Niterói. BR
  • Silva, Márcio Robert Mattos da; Federal University of Rio de Janeiro. Faculty of Pharmacy. Laboratório de Desenvolvimento Galênico. Rio de Janeiro. BR
  • Santos, Elisabete Pereira dos; Federal University of Rio de Janeiro. Faculty of Pharmacy. Laboratório de Desenvolvimento Galênico. Rio de Janeiro. BR
  • Ricci-Júnior, Eduardo; Federal University of Rio de Janeiro. Faculty of Pharmacy. Laboratório de Desenvolvimento Galênico. Rio de Janeiro. BR
Braz. J. Pharm. Sci. (Online) ; 58: e19175, 2022. tab, graf
Article de En | LILACS | ID: biblio-1374572
Bibliothèque responsable: BR40.1
Localisation: BR40.1
ABSTRACT
Abstract he aim of this work was to develop an oral solution of captopril at 5 mg/mL preservative-free. Two formulations were prepared, one containing sweetener (formulation 1) and the other without this excipient (formulation 2). The results found of validation parameters from analytical method performed by HPLC for captopril were, linearity 0.9998, the limit of detection 15.71 µg/mL, the limit of quantification 47.60 µg/mL, repeatability 1.05%, intermediate precision 2.42%, accuracy intraday 101,53%, accuracy inter-day 99.85%. Moreover, the results found for captopril disulfide were, linearity 0.9999, limit of detection 0.65 µg/mL, limit of quantification 1.96 µg/mL, repeatability 2.28%, intermediate precision 1.51%, accuracy intraday 101.36%, accuracy inter-day 100.29%. The appearance of formulations was clear and colorless, pH measures were 3.12 and 3.04, dosage of captopril and captopril disulfide were 99.45% and 99.82%, 0.24% and 0.12% for formulation 1 and formulation 2, respectively. The stability study demonstrated that the concentration of captopril and captopril disulfide in the formulations was > 90% and below 3%, respectively. The in vivo palatability study in animals and humans showed that Formulation 1 containing the sweetener had better acceptance. Thus, the sweetener was able to improve the unpleasant taste of the formulation
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Texte intégral: 1 Indice: LILACS Sujet Principal: Pédiatrie / Captopril / Chimie pharmaceutique / Stabilité de médicament langue: En Texte intégral: Braz. J. Pharm. Sci. (Online) Thème du journal: Farmacologia / Terapˆutica / Toxicologia Année: 2022 Type: Article

Texte intégral: 1 Indice: LILACS Sujet Principal: Pédiatrie / Captopril / Chimie pharmaceutique / Stabilité de médicament langue: En Texte intégral: Braz. J. Pharm. Sci. (Online) Thème du journal: Farmacologia / Terapˆutica / Toxicologia Année: 2022 Type: Article