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Research Article

Valuation of a Cellulose Acetate (CA) latex as coating material for controlled release products

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Pages 519-538 | Published online: 20 Oct 2008
 

Abstract

Cellulose acetate (CA) latex plasticized with 150% triacetin (TA) and 120% triethylcitrate (TEC), based on polymer weight, provided dense and homogeneous films when deposited onto propranolol HCl tablets using conventional fluid bed technology. Film permeability to the drug was low and flux/permeability enhancers were added to the CA structure during its manufacture. Films containing 40% surcrose and 10% PEG 8000 were found to provide the best release characteristics in terms of small lagtime (1 hour) and drug release profile (over 12 hours). When sucrose was added to TA or TEC plasticized fimls, a macroporous membrane was created during exposure to the dissolution fluid due to sucrose release from the film. These observations are consistent with the controlled porosity walls previously described for CA films deposited from organic solvents. It was postulated that drug mass transport occurs mainly within the porous CA structure and the mechanism responsible for its is a combination of molecular diffusion/osmotic pressure via water transport into the porous cellulose acetate membrane. Plasticizer loss during drying had also been demonstrated and related to the change in release profile seen with drying time.

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