Ednaldo Queiroga de Lima
Federal University of Campina Grande
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Pesquisa Veterinaria Brasileira | 2007
Ednaldo Queiroga de Lima; Miracy M. Albuquerque; Onaldo Guedes Rodrigues; José R.B. Alencar; Flávia Patrícia Morais de Medeiros; Pedro José Rolim Neto
Furosemide (40mg) was administered to 20 street dogs, 10 males and 10 females, in two different pharmaceutical forms: (1) compressed furosemide 40mg formulated at the Federal University of Pernambuco (UFPE-tablet), and (2) a commercial formulation with equal bioequivalence produced by the Laboratory for Pharmaceutical Technology of Pernambuco State (LAFEPE), the LAFEPE-furosemide. The study aimed to evaluate the kinetics of dissolution of the UFPE-tablet in order to analyze the behavior of bioavailability of the best formulation for veterinary use. The plasmatic concentrations of furosemide for the determination of parameters of pharmacological kinetics were analyzed by high-performance liquid chromatographic method (HPLC). The in vitro study accomplished through physiochemical analyses demonstrated that the formulas of the furosemide tablets attained the pharmaceutical requirements in agreement with USP 23 and the Brazilian Pharmacopoeia. The evaluation accomplished in dogs with UFPE-tablets given in only dose demonstrated uniformity in blood levels indicating stability in maintenance of the pharmaceutical formulation and efficiency in absorption of the active compound. These values are not significantly different in relation to the 5% confidence limit. Regarding maximum concentration (Tmax) time and global bioavaibility assessed by AUC means, there were no considerable differences as well. UFPE-furosemide displayed 743.492µg/mL.h as AUC average value whereas LAFEPE-furosemide had an average of 537.284µg/mL.h.Furosemide (40mg) was administered to 20 street dogs, 10 males and 10 females, in two different pharmaceutical forms: (1) compressed furosemide 40mg formulated at the Federal University of Pernambuco (UFPE-tablet), and (2) a commercial formulation with equal bioequivalence produced by the Laboratory for Pharmaceutical Technology of Pernambuco State (LAFEPE), the LAFEPE-furosemide. The study aimed to evaluate the kinetics of dissolution of the UFPE-tablet in order to analyze the behavior of bioavailability of the best formulation for veterinary use. The plasmatic concentrations of furosemide for the determination of parameters of pharmacological kinetics were analyzed by high-performance liquid chromatographic method (HPLC). The in vitro study accomplished through physiochemical analyses demonstrated that the formulas of the furosemide tablets attained the pharmaceutical requirements in agreement with USP 23 and the Brazilian Pharmacopoeia. The evaluation accomplished in dogs with UFPE-tablets given in only dose demonstrated uniformity in blood levels indicating stability in maintenance of the pharmaceutical formulation and efficiency in absorption of the active compound. These values are not significantly different in relation to the 5% confidence limit. Regarding maximum concentration (Tmax) time and global bioavaibility assessed by AUC means, there were no considerable differences as well. UFPE-furosemide displayed 743.492µg/mL.h as AUC average value whereas LAFEPE-furosemide had an average of 537.284µg/mL.h.
Acta Scientiarum. Health Science | 2006
Lívio César Cunha Nunes; Aíla Karla Mota Santana; José Lamartine Soares Sobrinho; Mônica Felts de La Roca; Ednaldo Queiroga de Lima; Pedro José Rolim Neto
Osteoporosis is a disease that affects a significant number of people in the world, particularly in developing countries. In this context, the powder of oyster shells, found to be a calcium source, emerges as one opportunity to use the natural resources from the Brazilian coast region for alimentary supplementation. This study proposes the use of this natural source of calcium, incorporated in tablets. The study was developed in two parts. The first was concerned with optimizing the raw material from oyster shells, from the selection process until the transformation of de oyster shell into dust; and with the physicochemical evaluation and preformulation of this dust. The second part consisted of obtaining tablets, from the development until the comparative evaluation of lyoavailability. The studies on preformulation and factorial planning of the excipients (binging agent, levigating agent and disintegrants) have made possible to obtain tables with a similar lyoavailability, in terms of economy and performance, to the medicine reference Os-cal ®
AGROPECUÁRIA CIENTÍFICA NO SEMIÁRIDO | 2010
VMaria do Socorro Vieira Pereira; Onaldo Guedes Rodrigues; Francisco Marlon Carneiro Feijó; Ana Célia Rodrigues Athayde; Ednaldo Queiroga de Lima; Maria Raquel Querino de Sousa
Archive | 2007
Mônica Felts de La Roca; Ednaldo Queiroga de Lima; Pedro J. Rolim-Neto; Artur de Sá
Agropecuária Técnica | 2010
Luiz Feranando Annunziata Trevisan; Márcia Almeida de Melo; Andréia Vieira Pereira; Ednaldo Queiroga de Lima; Onaldo Guedes Rodrigues; Maria do Socorro Vieira Pereira; Ana Carolina Lyra de Albuquerque
Agropecuária Técnica | 2010
Andréia Vieira Pereira; Luiz Feranando Annunziata Trevisan; Onaldo Guedes Rodrigues; Laura Ney Marcelino Passerat Silans; Márcia Almeida de Melo; Ednaldo Queiroga de Lima; Nilton Guedes do Nascimento Junior; Maria do Socorro Vieira Pereira
Agropecuária Técnica | 2009
Luiz Feranando Annunziata Trevisan; Andréia Vieira Pereira; Ana Carolina Lyra de Albuquerque; Maria do Socorro Vieira Pereira; Jozinete Vieira Pereira; Onaldo Guedes Rodrigues; Ednaldo Queiroga de Lima; Márcia Almeida de Melo
Rev. ciênc. farm | 2004
L. R. P Lima; T. T Oliveira; T. J Nagem; Ednaldo Queiroga de Lima; P Rolim Neto
Buffalo Bulletin | 2017
Andréia Vieira Pereira; Marcelo Biondaro Góis; Fabiana Nabarro Ferraz; Jozinete Vieira Pereira; Sérgio Santos de Azevedo; Ednaldo Queiroga de Lima; Onaldo Guedes Rodrigues; Elizabeth Sampaio de Medeiros; Rinaldo Aparecido Mota; Maria do Socorro Vieira Pereira
Agropecuária Técnica | 2010
Andréia Vieira Pereira; Luiz Feranando Annunziata Trevisan; Tatiane Kelly Barbosa de Azevêdo; Karla Aparecida Oliveira; Severino Silvano Dos Santos Higino; Maria Regina Macedo Costa; Maria do Socorro Vieira Pereira; Onaldo Guedes Rodrigues; Ednaldo Queiroga de Lima