Literature DB >> 19763838

Ethyl cellulose microcapsules for protecting and controlled release of folic acid.

Satit Prasertmanakit1, Nalena Praphairaksit, Worawadee Chiangthong, Nongnuj Muangsin.   

Abstract

Ethyl cellulose microcapsules were developed for use as a drug-delivery device for protecting folic acid from release and degradation in the undesirable environmental conditions of the stomach, whilst allowing its release in the intestinal tract to make it available for absorption. The controlled release folic acid-loaded ethyl cellulose microcapsules were prepared by oil-in-oil emulsion solvent evaporation using a mixed solvent system, consisting of a 9:1 (v/v) ratio of acetone:methanol and light liquid paraffin as the dispersed and continuous phase. Span 80 was used as the surfactant to stabilize the emulsion. Scanning electron microscopy revealed that the microcapsules had a spherical shape. However, the particulate properties and in vitro release profile depended on the concentrations of the ethyl cellulose, Span 80 emulsifier, sucrose (pore inducer), and folic acid. The average diameter of the microcapsules increased from 300 to 448 microm, whilst the folic acid release rate decreased from 52% to 40%, as the ethyl cellulose concentration was increased from 2.5% to 7.5% (w/v). Increasing the Span 80 concentration from 1% to 4% (v/v) decreased the average diameter of microcapsules from 300 to 141 microm and increased the folic acid release rate from 52% to 79%. The addition of 2.5-7.5% (w/v) of sucrose improved the folic acid release from the microcapsules. The entrapment efficiency was improved from 64% to 88% when the initial folic acid concentration was increased from 1 to 3 mg/ml.

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Year:  2009        PMID: 19763838      PMCID: PMC2799571          DOI: 10.1208/s12249-009-9305-3

Source DB:  PubMed          Journal:  AAPS PharmSciTech        ISSN: 1530-9932            Impact factor:   3.246


  14 in total

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2.  Oral sustained-release drug delivery systems using polycarbonate microspheres capable of floating on the gastric fluid.

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3.  Folate and folate-binding protein content in dairy products.

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4.  Effect of viscosity and concentration of wall former, emulsifier and pore-inducer on the properties of amoxicillin microcapsules prepared by emulsion solvent evaporation.

Authors:  Mingna Song; Ning Li; Shuying Sun; Lourens R Tiedt; Wilna Liebenberg; Melgardt M de Villiers
Journal:  Farmaco       Date:  2005-03

5.  In vitro modified release of acyclovir from ethyl cellulose microspheres.

Authors:  S J Cheu; R R Chen; P F Chen; W J Lin
Journal:  J Microencapsul       Date:  2001 Sep-Oct       Impact factor: 3.142

6.  Preparation of non-porous microspheres with high entrapment efficiency of proteins by a (water-in-oil)-in-oil emulsion technique.

Authors:  N B Viswanathan; P A Thomas; J K Pandit; M G Kulkarni; R A Mashelkar
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8.  Identification of photoproducts of folic acid and its degradation pathways in aqueous solution.

Authors:  M Jamil Akhtar; M Ataullah Khan; Iqbal Ahmad
Journal:  J Pharm Biomed Anal       Date:  2003-03-10       Impact factor: 3.935

9.  Preparation and characterization of ethylcellulose microspheres containing 5-fluorouracil.

Authors:  C Zinutti; F Kedzierewicz; M Hoffman; P Maincent
Journal:  J Microencapsul       Date:  1994 Sep-Oct       Impact factor: 3.142

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Authors:  K Suzuki; J C Price
Journal:  J Pharm Sci       Date:  1985-01       Impact factor: 3.534

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3.  Application of Ethyl Cellulose and Ethyl Cellulose + Polyethylene Glycol for the Development of Polymer-Based Formulations using Spray-Drying Technology for Retinoic Acid Encapsulation.

Authors:  Antónia Gonçalves; Fernando Rocha; Berta N Estevinho
Journal:  Foods       Date:  2022-08-22

4.  Ultrahigh verapamil-loaded controlled release polymeric beads using superamphiphobic substrate: D-optimal statistical design, in vitro and in vivo performance.

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  4 in total

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