For Libraries For Publication Open Access Downloads About Us Contact Us
Paper Titles
Effect of Galactomannan on the Dynamic Properties of Xyloglucan Aqueous Solution
p.266
Determination of Surface Free Energy and Contact Angle for Hydrolyzed Shellac
p.270
Comparison of In Vitro Binding of Bile Salt by Pectins from Various Sources
p.274
Thermal Analysis of Chitosan-Lactate and Chitosan-Aluminum Monostearate Composite System
p.278
Drug-Loaded Pectin Microparticles Prepared by Emulsion-Solvent Evaporation
p.282
Pectin-Based Nano-Sized Emulsions Prepared by High-Pressure Homogenization
p.286
Design of Shellac-Based Film with Improved Mechanical Properties through Composite Formation with Clay
p.290
Effect of Ultrasonic Treatment on Physical Properties of Tapioca Starch
p.294
Heterocoaggulation of Natural Rubber Latex and Poly [Styrene-co-2-(Methacryloyloxy) Ethyl Trimethylammonium Chroride] Nanoparticles
p.299

Drug-Loaded Pectin Microparticles Prepared by Emulsion-Solvent Evaporation

Article Preview

Abstract:

The aim of this study was to develop the pectin-based microparticles by emulsion-solvent evaporation technique. The effects of concentration and type of pectin and addition of glutaraldehyde on size, size distribution, drug crystalline state and drug dissolution from microparticles were investigated. The results showed that a model drug, indomethacin, could be encapsulated in microparticles. Higher molecular weight of pectin caused a larger in size of microparticles than the lower one. A high degree of esterification is preferred to stabilize the pectin microparticles. The powder x-ray diffractograms showed that all microparticles led to amorphous products while their physical mixture still showed the crystalline state of drug. Drug dissolution from the microparticles containing indomethacin and pectin was increased, resulting from the formation of an amorphous solid dispersion. Addition of glutaraldehyde, however, resulted in slower drug dissolution, compared to the formulations without glutaraldehyde or drug alone.

You might also be interested in these eBooks
Biomaterials and Applications View Preview

Info:

Periodical:

Advanced Materials Research (Volume 506)

Pages:

282-285

DOI:

https://doi.org/10.4028/www.scientific.net/AMR.506.282

Citation:

Cite this paper

Online since:

April 2012

Authors:

Pornsak Sriamornsak, S. Konthong, K. Burapapadh, Srisagul Sungthongjeen

Keywords:

Emulsion-Solvent Evaporation, Microparticles, Pectin, Solid Dispersion

Export:

RIS, BibTeX

Price:

Permissions CCC:

Request Permissions

Permissions PLS:

Request Permissions

Сopyright:

© 2012 Trans Tech Publications Ltd. All Rights Reserved

Share:

Citation:

References

[1] G.G. Liversidge, K.C. Cundy: Int J Pharm, Vol. 125(1995), p.91.

Google Scholar

[2] P. Sriamornsak: Silpakorn U Int J, Vol. 3(2003), p.206.

Google Scholar

[3] P. Sriamornsak: Expert Opin Drug Del, Vol. 8(2011), p.1009.

Google Scholar

[4] K. Burapapadh, M. Kumpugdee-Vollrath, D. Chantasart, P. Sriamornsak: Carbohydr Polym, Vol. 82(2010), p.385.

DOI: 10.1016/j.carbpol.2010.04.071

Google Scholar

© 2025 Trans Tech Publications Ltd. All rights are reserved, including those for text and data mining, AI training, and similar technologies. For open access content, terms of the Creative Commons licensing CC-BY are applied.
Scientific.Net is a registered trademark of Trans Tech Publications Ltd.