Effect of antioxidants on captopril floating matrices

Inéz Jiménez-Martnez, Adriana Miriam Domnguez-Ramrez, Leopoldo Villafuerte-Robles

Research output: Contribution to journalArticlepeer-review

6 Scopus citations

Abstract

Stability of captopril in a controlled release formulation has been a challenge for some time. The sustained release of captopril from floating matrices has been studied varying the antioxidant load, the sodium bicarbonate proportion and the compaction pressure. Although in many cases the effect of compaction pressure remains hidden, actual results show that matrices compacted at 55MPa have smaller density and float in the dissolution medium while those compacted at 165MPa float only adding sodium bicarbonate. The increase of compaction pressure reduces the hydration volume and increases the time necessary to attain its maximum. These changes are attributed to lower matrix porosity and to the consequent diminution of water and drug transport. Increasing ascorbic acid proportions increase the matrix hydration volume and the drug released. The use of sodium ascorbate and the substitution of 15% polymer with sodium bicarbonate reduce the matrix hydration volume, shorten the matrix hydration process and increase the drug released. This is attributed to carbon dioxide bubbles that decrease the matrix coherence and expand the matrix volume, facilitating drug dissolution and only a limited further matrix expansion. The antioxidant protection provided by sodium ascorbate was lesser of that of ascorbic acid because of greater molecular mass and lesser release rate.

Original languageEnglish
Pages (from-to)230-240
Number of pages11
JournalPharmaceutical Development and Technology
Volume15
Issue number3
DOIs
StatePublished - Jun 2010

Keywords

  • Antioxidants
  • Captopril floating tablets
  • Compaction pressure
  • Hydration kinetics
  • Hydroxypropyl methylcellulose

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