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Please use this identifier to cite or link to this item: http://142.54.178.187:9060/xmlui/handle/123456789/12833
Title: Biowaiver studies of Metronidazole tablets (400mg): An alternative to In-vivo bioequivalence Studies
Authors: Safdar, Kashif Ali
Naqvi, Syed Baqir
Usman, Shahnaz
Rehman, Saeed-ur-
Muhammad, Iyad Naeem
Keywords: Metronidazole
dissolution behavior
comparative study
biowaiver studies
Issue Date: Nov-2018
Publisher: Pakistan Journal of Pharmaceutical Sciences University of Karachi
Citation: Safdar, K. A., Naqvi, S. B., Usman, S., & Muhammad, I. N. (2018). Biowaiver studies of Metronidazole tablets (400mg): An alternative to In-vivo bioequivalence Studies. Pakistan Journal of Pharmaceutical Sciences, 31(6).
Abstract: The aim of the study was to investigate the dissolution behavior of commercially available brands of metronidazole and to provide basic tool to evaluate the comparative effectiveness and interchangeability of generic brands under biowaiver conditions. The dissolution test for six brands of metronidazole 400mg tablets was performed and physical controls were analyzed. Basket Rack methods at 100rpm were used to estimate release pattern of drug. Pharmaceutical parameters of tablets were analyzed. In order to evaluate dissolution profiles, multiple point dissolution were performed and calculated 85.96±0.41 to 90.56±0.93 % within 15 minutes in pH 1.2,85.50±1.40 to 88.99±0.80% in pH 4.5 and 85.37±1.94 to 92.79±0.89% in pH 6.8 dissolution medium respectively. Five different kinetics have been studied to predict and evaluate the acceptability level of drug release. The results show that Hixson-Crowell, first-order and Weibull demonstrated the drug release with R2 ≥ 0.95 that predicted the tablets were pharmaceutically equivalent. One-way ANOVA at p ≥0.05 level and similarity factors (f2) were used to estimate the discrepancy and intimacy among the brands. It is a need of time to constantly monitor the marketed generic drugs products and their release profiles to confirm their in vitro bioequivalence which can help to reduce the time, cost and unnecessary exposure of healthy subjects to medicines.
URI: http://142.54.178.187:9060/xmlui/handle/123456789/12833
ISSN: 1011-601X
Appears in Collections:Issue 6

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