AI Article Synopsis

  • The text discusses the need to treat peptic and duodenal ulcers caused by a common bacterium, with a focus on delivering metronidazole effectively.
  • Scientists developed floating tablets that release metronidazole gradually, using cellulose and Avicel, resulting in a slower release compared to conventional tablets.
  • In vivo studies showed these floating tablets improved drug absorption and sustained release, offering a potentially more effective treatment method for ulcer-related conditions.

Article Abstract

is thought to be the most common cause of peptic and duodenal ulcers. Eradication of this organism is now considered one of the lines of treatment of gastric and duodenal ulcers. This can be achieved via local delivery of antibacterial agents in high concentrations. Accordingly, our objective was to fabricate and evaluate sustained release floating tablets for metronidazole to extend the gastric residence period and control the release rate of metronidazole. Floating tablets containing cellulose derivatives and Avicel were prepared using direct compression. The rate of metronidazole release from the floating tablets (K = 6.278 mg min) was significantly lower than that from conventional tablets (K = 10.666 mg min), indicating sustained drug release, according to the Higuchi model, for more than 6 h in an acidic medium of 0.1 N HCl. In vivo study in healthy volunteers revealed significantly improved bioavailability; increased Tmax, AUC, and MRT; and significantly lower absorption rate constant after a single oral dose of 150 mg metronidazole as floating tablets. In addition, the significant increase in MRT indicated an in vivo sustained drug release. The floating tablets provided several benefits, including ease of preparation, absence of effervescent ingredients, and reliance on a pH-independent gel-forming agent to deliver metronidazole in a sustained manner. In conclusion, the prepared tablets could be promising for enhancing both local and systemic metronidazole efficacy.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9024553PMC
http://dx.doi.org/10.3390/pharmaceutics14040863DOI Listing

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