AI Article Synopsis

  • - This study developed a floating raft system to deliver etoricoxib (ETO) and famotidine (FAM) using polysaccharides like glucomannan, focusing on factors like gelation and release time.
  • - The optimal formulation included specific percentages of ingredients, resulting in fast gelation and floating times while allowing controlled drug release over 8 hours.
  • - X-ray studies confirmed the raft's buoyancy for about 8 hours and showed that this new system had better bioavailability compared to existing products, indicating effective dual drug delivery.

Article Abstract

This study aimed to formulate and evaluate a floating raft system for the co-delivery of etoricoxib (ETO) and famotidine (FAM) using a combination of glucomannan with natural/semi-synthetic polysaccharides. Formulation variables affect gelation lag time (GLT), floating lag time (FLT), and release percentage of drugs after 1-8 h, Stability, and viscosity parameters were evaluated. In vivo X-ray studies, followed by the pharmacokinetic study, were performed on human volunteers. Formulations exhibited pseudoplastic behavior for ease of swallowing. The optimum raft system (ORS) comprised 1% Na alginate, 0.1% Low Methoxyl (LM) pectin, 0.8% Konjac glucomannan (KGL), 1% Precirol, and 1% CaCO. ORS exhibited rapid GLT and FLT (around 42 and 8 sec respectively) in 0.1 N HCl as well as controlled release of ETO (15% in 1 h and 82% in 8 h) and FAM (29% in 1 h and 85% in 8 h). Formulation stability with the absence of any drug-excipient interactions was observed. The X-ray imaging showed a promising buoyancy ability for approximately 8 h. Compared with marketed products, ORS showed superior relative bioavailability for both drugs. These findings revealed the successful preparation of a promising raft system with improved dual drug delivery.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10184610PMC
http://dx.doi.org/10.1080/10717544.2023.2189630DOI Listing

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