Analysis of spironolactone polymorphs in active pharmaceutical ingredients and their effect on tablet dissolution profiles

Authors

  • Renata Cunha de Resende Federal University of Alfenas; Faculty of Pharmaceutical Sciences; Department of Pharmacy
  • Olímpia Maria Martins Santos Viana Federal University of Alfenas; Faculty of Pharmaceutical Sciences; Department of Pharmacy
  • Jennifer Tavares Jacon Freitas Federal University of Alfenas; Faculty of Pharmaceutical Sciences; Department of Pharmacy
  • Rudy Bonfilio Federal University of Alfenas; Faculty of Pharmaceutical Sciences; Department of Pharmacy
  • André Luís Morais Ruela Federal University of Bahia; Multidisciplinary Health Institute
  • Magali Benjamim de Araújo Federal University of Alfenas; Faculty of Pharmaceutical Sciences; Department of Pharmacy

DOI:

https://doi.org/10.1590/s1984-82502016000400005

Abstract

Spironolactone (SPR) is a steroidal drug administered as a potassium-sparing diuretic for high blood pressure treatment. The drug shows incomplete gastrointestinal absorption due to its poor aqueous solubility. The physicochemical properties of SPR in crystal forms I and II suggest that differences in their aqueous solubility may lead to a lack of bioequivalence between solid-state formulations. In this study, SPR polymorphs in five batches of active pharmaceutical ingredients (APIs) from three manufacturers were characterized using powder X-ray diffraction, infrared spectroscopy, thermal analysis, and solubility measurements. SPR tablets (50 mg) were manufactured in our laboratory using API in pure form II, and API in form II contaminated with form I, which was found in a commercial batch. Physicochemical quality evaluations of the manufactured tablets, along with five SPR tablets marketed in Brazil, were performed, and results indicated differences in their dissolution profiles. In the manufactured tablets, differences were associated with the increased solubility of API in form II contaminated with form I compared to API in pure form II. In the marketed SPR tablets, the formulation composition demonstrated an important role in the dissolution rate of the drug, leading to lack of pharmaceutical equivalence among the drug products.

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Published

2016-12-01

Issue

Vol. 52 No. 4 (2016)

Section

Articles

License

All content of the journal, except where identified, is licensed under a Creative Commons attribution-type BY.

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How to Cite

Analysis of spironolactone polymorphs in active pharmaceutical ingredients and their effect on tablet dissolution profiles . (2016). Brazilian Journal of Pharmaceutical Sciences, 52(4), 613-621. https://doi.org/10.1590/s1984-82502016000400005