Determinação do perfil farmacocinético de anti-inflamatórios não hormonais aplicados à clinica / Determination of the pharmacokinetic profile of the non-steroidal anti-inflammatory drugs related with clinic outcomes
AUTOR(ES)
Hamilton Modesto Rigato
FONTE
IBICT - Instituto Brasileiro de Informação em Ciência e Tecnologia
DATA DE PUBLICAÇÃO
12/08/2011
RESUMO
Objective: The present work aims to evaluation the pharmacokinetic profile of the diclofenac-cholestyramine (140mg capsule) and two pharmaceuticals formulations (100mg tablets and 50mg/m oral suspension) of nimesulide in healthy adult subjects related with clinic outcomes in the hepatic enzymes panel and platelet count. Method: The studies were open, randomized, simple crossover balanced with two periods. The blood samples were analyzed by high performance liquid chromatography coupled to ultraviolet detection in diclofenac formulations. For nimesulide a mass espectrometer was performed (MS/MS). Seric enzymes from liver panels and whole blood platelet count was compared with pre and post single dose treatment. Results: The geometric mean and 90% confidence intervals (CI) for the diclofenac-cholestyramine/Flotac® ratio were 100.22% (84.99 - 118.19%) for CMAX and 90,53% (82.86-98.91%) for AUCLAST. The geometric mean and 90% confidence intervals (CI) for the Nimesulide/Nisulid® 100mg tablet were 85.96% (77.54 - 95.30%) for CMAX and 93.91% (84.42 - 104.46%) for AUCLAST, and for the oral suspension 50mg/mL were 100.1% (91.05 - 110.15%) for CMAX and 107.7% (99.74 - 116.39%) for AUCLAST. For the hepatic enzyme panel was observed significant rise in the ALT for diclofenac-cholestyramine and nimesulide tablet. The oral suspension was significant rise in the ALP parameter (p<0.05). No platelet count decrease was observed. Conclusion: Since the 90% CI for CMAX and AUCLAST ratios were all inside the 80-125% interval proposed by the US Food and Drug Administration and accepted by ANVISA, it is concluded that the diclofenac-cholestyramine 140mg capsule and the nimesulide oral suspension formulation 50mg/mL are bioequivalent in regard to both extent and rate of absorption. The nimesulide 100mg tablet is not bioequivalent to Nisulid® 100mg tablet with respect to the rate of absorption. Clinically all the evaluated pharmaceuticals are safety despide the significant changes in the hepatic enzymes panel observed
ASSUNTO(S)
farmacocinética antiinflamatórios não esteróides cromatografia líquida toxicidade de drogas pharmacokinetics anti-inflammatory agents non-steroidal chromatography liquid drug toxicity
