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Formulation of dacarbazine-loaded Cubosomes--part II: influence of process parameters. | LitMetric

Formulation of dacarbazine-loaded Cubosomes--part II: influence of process parameters.

AAPS PharmSciTech

Division of Pharmaceutical Sciences, University of Missouri-Kansas City School of Pharmacy, Kansas City, Missouri 64110-2499, USA.

Published: February 2010

AI Article Synopsis

  • The study examines how different process parameters like homogenization speed, duration, and temperature affect the creation of dacarbazine-loaded cubosomes, focusing on particle size and encapsulation efficiency.
  • Box-Behnken design was used to analyze these variables, leading to a polynomial model that helps predict outcomes and optimize conditions for better results.
  • The optimal settings determined were approximately 24,000 rpm speed, 5.5 minutes, and 76 degrees Celsius, yielding cubosomes with a particle size of 85.6 nm and 16.7% encapsulation efficiency, although further research is required to improve encapsulation efficiency.

Article Abstract

The purpose of this study is to investigate the combined influence of process parameters (independent variables) such as homogenization speed (X(1)), duration (X(2)), and temperature (X(3)) during the preparation of dacarbazine-loaded cubosomes. Box-Behnken design was used to rationalize the influence of these three factors on two responses, namely particle size (Y(1)) and encapsulation efficiency (Y(2)). Independent and dependent variables were analyzed with multiple regressions to establish a full-model second-order polynomial equation. F value was calculated to confirm the omission of insignificant parameters or interactions of parameters from the analysis to derive a reduced-model polynomial equation to predict the Y(1) and Y(2) of dacarbazine-loaded cubosomes. Pareto charts were also obtained to show the effects of X(1), X(2), and X(3) on Y(1) and Y(2). For Y(1), there was a model validated for more accurate prediction of response parameter by performing checkpoint analysis. The optimization process and Pareto charts were obtained automatically and they predicted the levels of independent parameters X(1), X(2), and X(3) (0.889794, 0.11886, and 0.56201, respectively) and minimized Y(1). The optimal process parameters (homogenization's speed = approximately 24,000 rpm, duration = 5.5 min, and temperature = 76 degrees C) led to the production of cubosomes with 85.6 nm in size and 16.7% in encapsulation efficiency. The Box-Behnken design proved to be a useful tool in the preparation and optimization of dacarbazine-loaded cubosomes. For encapsulation efficiency (Y(2)), further studies are needed to enhance the result and improve the model for such water-soluble drug encapsulation in cubosomes.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2802167PMC
http://dx.doi.org/10.1208/s12249-009-9296-0DOI Listing

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