Solid dispersions with hydrogenated castor oil increase solubility, dissolution rate and intestinal absorption of praziquantel

Authors

  • Marco Vinicius Chaud Methodist University of Piracicaba; Faculty of Health Sciences; Department of Pharmacy
  • Pollyanna Tamascia Methodist University of Piracicaba; Faculty of Health Sciences; Department of Pharmacy
  • Andréa Cristina de Lima São Paulo State University Júlio de Mesquita Filho; Faculty of Pharmaceutical Sciences; Department of Drugs and Pharmaceutical
  • Maria Ondina Paganelli Methodist University of Piracicaba; Faculty of Health Sciences; Department of Pharmacy
  • Maria Palmira Daflon Gremião São Paulo State University Júlio de Mesquita Filho; Faculty of Pharmaceutical Sciences; Department of Drugs and Pharmaceutical
  • Osvaldo de Freitas University of São Paulo; Department of Pharmaceutical Sciences

DOI:

https://doi.org/10.1590/S1984-82502010000300010

Keywords:

Solid dispersion, Praziquantel^i1^sdissolution ra, Praziquantel^i1^ssolubil, Praziquantel^i1^sintestinal absorpt

Abstract

The solubility behavior of drugs remains one of the most challenging aspects in formulation development. Solid Dispersion (SD) has tremendous potential for improving drug solubility. Although praziquantel (PZQ) is the first drug of choice in the treatment of schistosomiasis, its poor solubility has restricted its delivery oral route. In spite of its poor solubility, PZQ is well absorbed in the gastrointestinal tract, but large doses are required to achieve adequate concentration at the target sites. The aim of this study was to improve the solubility and dissolution rate of PZQ and to evaluate its intestinal absorption. SDs were formulated with PEG-60 castor oil hydrogenated (CR-60) using a fusion and evaporation method. Pure PZQ and physical mixtures (PM) and PZQ-CR-60 (2:1; 1:1; 1:2 ratios) were compared as regards their solubility, dissolution and intestinal absorption. The experimental results demonstrated the improvement in the solubility, dissolution rate and intestinal absorption. In addition, the solubility behavior showed pH dependency and that the solubility of PZQ was slower in acidic medium than in neutral and basic mediums. The increase in PZQ solubility of the SD with the CR-60 could be attributed to several factors such as improved wettability, local solubilization, drug particle size reduction and crystalline or, interstitial solid solution reduction.

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Published

2010-09-01

Issue

Section

Original Papers

How to Cite

Solid dispersions with hydrogenated castor oil increase solubility, dissolution rate and intestinal absorption of praziquantel . (2010). Brazilian Journal of Pharmaceutical Sciences, 46(3), 473-481. https://doi.org/10.1590/S1984-82502010000300010