Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
2485105 | Journal of Pharmaceutical Sciences | 2010 | 11 Pages |
Abstract
Considerable interest has been focused on curcumin due to its use to treat a wide variety of disorders, however, the therapeutic potential of curcumin could often be limited by its poor solubility, bioavailability, and photostability. To overcome these drawbacks, efficacious formulations of curcumin, including nanocrystal solid dispersion (CSDâCur), amorphous solid dispersion (ASDâCur), and nanoemulsion (NEâCur), were designed with the aim of improving physicochemical and pharmacokinetic properties. Physicochemical properties of the prepared formulations were characterized by scanning/transmission electron microscope for morphological analysis, laser diffraction, and dynamic light scattering for particle size analysis, and polarized light microscope, powder Xâray diffraction and differential scanning calorimetry for crystallinity assessment. In dissolution tests, all curcumin formulations exhibited marked improvement in the dissolution behavior when compared with crystalline curcumin. Significant improvement in pharmacokinetic behavior was observed in the newly developed formulations, as evidenced by 12â (ASDâCur), 16â (CSDâCur), and 9âfold (NEâCur) increase of oral bioavailability. Upon photochemical characterization, curcumin was found to be photoreactive and photodegradable in the solution state, possibly via type 2 photochemical reaction, whereas high photochemical stability was seen in the solid formulations, especially CSDâCur. On the basis of these observations, taken together with dissolution and pharmacokinetic behaviors, CSD strategy would be efficacious to enhance bioavailability of curcumin with high photochemical stability. © 2009 WileyâLiss, Inc. and the American Pharmacists Association J Pharm Sci 99: 1871-1881, 2010
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Authors
Satomi Onoue, Haruki Takahashi, Yohei Kawabata, Yoshiki Seto, Junya Hatanaka, Barbara Timmermann, Shizuo Yamada,