Preparation of curcumin self-micelle solid dispersion with enhanced bioavailability and cytotoxic activity by mechanochemistry

Qihong Zhang; Nikolay E. Polyakov; Yulia S. Chistyachenko; Mikhail V. Khvostov; Tatjana S. Frolova; Tatjana G. Tolstikova; Alexandr V. Dushkin; Weike Su

doi:10.1080/10717544.2017.1422298

Drug Delivery (Jan 2018)

Preparation of curcumin self-micelle solid dispersion with enhanced bioavailability and cytotoxic activity by mechanochemistry

Qihong Zhang,
Nikolay E. Polyakov,
Yulia S. Chistyachenko,
Mikhail V. Khvostov,
Tatjana S. Frolova,
Tatjana G. Tolstikova,
Alexandr V. Dushkin,
Weike Su

Affiliations

Qihong Zhang: National Engineering Research Center for Process Development of Active Pharmaceutical Ingredients, Collaborative Innovation Center of Yangtze River Delta Region Green Pharmaceuticals, Zhejiang University of Technology
Nikolay E. Polyakov: Institute of Chemical Kinetics and Combustion
Yulia S. Chistyachenko: Institute of Solid State Chemistry and Mechanochemistry
Mikhail V. Khvostov: N.N. Vorozhtsov Institute of Organic Chemistry SB RAS
Tatjana S. Frolova: N.N. Vorozhtsov Institute of Organic Chemistry SB RAS
Tatjana G. Tolstikova: N.N. Vorozhtsov Institute of Organic Chemistry SB RAS
Alexandr V. Dushkin: Institute of Solid State Chemistry and Mechanochemistry
Weike Su: National Engineering Research Center for Process Development of Active Pharmaceutical Ingredients, Collaborative Innovation Center of Yangtze River Delta Region Green Pharmaceuticals, Zhejiang University of Technology

DOI: https://doi.org/10.1080/10717544.2017.1422298
Journal volume & issue: Vol. 25, no. 1
pp. 198 – 209

Abstract

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An amorphous solid dispersion (SD) of curcumin (Cur) with disodium glycyrrhizin (Na2GA) was prepared by mechanical ball milling. Curcumin loaded micelles were self-formed by Na2GA when SD dissolved in water. The physical properties of Cur SD in solid state were characterized by differential scanning calorimetry, X-ray diffraction studies, and scanning electron microscope. The characteristics of the sample solutions were analyzed by reverse phase HPLC, UV–visible spectroscopy, 1H NMR spectroscopy, gel permeation LC, and transmission electron microscopy. In vitro cytotoxic tests demonstrated that Cur SD induced higher cytotoxicity against glioblastoma U-87 MG cells than free Cur. Besides, an improvement of membrane permeability of Cur SD was confirmed by parallel artificial membrane permeability assay. Further pharmacokinetic study of this SD formulation in rat showed a significant ∼19-fold increase of bioavailability as comparing to free Cur. Thus, Cur SD provide a more potent and efficacious formulation for Cur oral delivery.

Published in Drug Delivery

ISSN: 1071-7544 (Print); 1521-0464 (Online)
Publisher: Taylor & Francis Group
Country of publisher: United Kingdom
LCC subjects: Medicine: Therapeutics. Pharmacology
Website: https://www.tandfonline.com/journals/idrd

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