4.4 Article

Binary lipids-based nanostructured lipid carriers for improved oral bioavailability of silymarin

Journal

JOURNAL OF BIOMATERIALS APPLICATIONS
Volume 28, Issue 6, Pages 887-896

Publisher

SAGE PUBLICATIONS LTD
DOI: 10.1177/0885328213485141

Keywords

Nanostructured lipid carrier; silymarin; glycerol distearate; oleic acid; oral bioavailability

Funding

  1. National Key Basic Research Program of China [2009CB930300]
  2. Shanghai Municipal Commission of Education [10SG05]
  3. Ministry of Education [NCET-11-0114]

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The main purpose of this study was to prepare binary lipids-based nanostructured lipid carriers to improve the oral bioavailability of silymarin, a poorly water-soluble liver protectant. Silymarin-loaded nanostructured lipid carriers were prepared by the method of high-pressure homogenization with glycerol distearates (Precirol ATO-5) and oleic acid as the solid and liquid lipids, respectively, and lecithin (Lipoid E 100) and Tween-80 as the emulsifiers. The silymarin-nanostructured lipid carrier prepared under optimum conditions was spherical in shape with mean particle size of approximate to 78.87nm, entrapment efficiency of 87.55%, loading capacity of 8.32%, and zeta potential of -65.3mV, respectively. Invitro release of silymarin-nanostructured lipid carriers was very limited even after 12h, while invitro lipolysis showed fast digestion of nanostructured lipid carriers within 1h. Relative oral bioavailability of silymarin-nanostructured lipid carriers in Beagle dogs was 2.54- and 3.10-fold that of marketed Legalon (R) and silymarin solid dispersion pellets, respectively. It was concluded that nanostructured lipid carriers were potential drug delivery systems to improve the bioavailability of silymarin. Other than improved dissolution, alternative mechanisms such as facilitated absorption as well as lymphatic transport may contribute to bioavailability enhancement.

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