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Chitosan–alginate multilayer beads for controlled release of ampicillin .pdf
International Journal of Pharmaceutics 290 (2005) 45–54
Chitosan–alginate multilayer beads for controlled
release of ampicillin
∗
Anil K. Anal , Willem F. Stevens
Bioprocess Technology Program, Asian Institute of Technology, Klong Luang, Bangkok 12120, Thailand
Received 20 August 2004; received in revised form 12 November 2004; accepted 15 November 2004
Available online 5 January 2005
Abstract
The aim of this study is to develop multilayer beads with improved properties for controlled delivery of the antibiotic
ampicillin. Ionotropic gelation was applied to prepare single and multilayer beads using various combinations of chitosan and
Ca2+ as cationic components and alginate and polyphosphate as anions. Beads prepared with higher concentrations of chitosan
entrapped more ampicillin. During incubation in simulated gastric fluid, the beads swelled and started to float but did not show
any sign of erosion. Single layer chitosan–alginate beads released 70% of the drug within 4 h. Multilayer beads released only
20–30% in the same period of time. During subsequent incubation in simulated intestinal fluid, both single and multilayer beads
continued to release drug. At least part of this release is due to disintegration of the beads. The rate of release both in gastric
and intestinal fluid and the kinetics of disintegration in intestinal fluid can be controlled by changing the chitosan concentration
in the coagulation fluid. The release of the drug can also be controlled by the degree of cross-linking using polyphosphate.
Cross-linked multilayer beads were prepared that released only 40% of the entrapped drug during 24 h. It is concluded
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