Membrane Permeation-Controlled Transdermal Delivery System Design. Influence of Controlling Membrane and Adhesive on Skin Permeation of Isosorbide Dinitrate

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Abstract

A membrane permeation-controlled transdermal delivery system (MC-TDS) of isosorbide dinitrate (ISDN), a model drug, was prepared from polyvinyl alcohol aqueous gel containing the drug, a membrane consisting of ethylene-vinyl acetate copolymer membrane and acrylic adhesive (EV-a). The permeability of ISDN through the EV-a membrane was 2.5 times higher than that through excised hairless rat skin. The ratio of plasma concentration of ISDN after application of MC-TDS on stripped (damaged) skin relative to intact skin was lower than that after application of Frandol tape-S, a marketed ISDN TDS, which suggests that the EV-a membrane might work as a control membrane for overall delivery rate of ISDN to the body. When MC-TDS stored at 30 °C for 13.5-48 h was applied to the damaged skin, however, the initial plasma concentration of ISDN was very much higher than the expected therapeutic level and was not controlled by the EV-a membrane. The initial high plasma concentration of ISDN after application of the stored MC-TDS on the damaged skin was due to migration of ISDN from the reservoir to the adhesive during storage at 30 °C. The migration of drugs into the adhesive might be an important problem in developing efficient MC-TDS. © 1990, The Pharmaceutical Society of Japan. All rights reserved.

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APA

Seki, T., Kawaguchi, T., Sugibayashi, K., Juni, K., & Morimoto, Y. (1990). Membrane Permeation-Controlled Transdermal Delivery System Design. Influence of Controlling Membrane and Adhesive on Skin Permeation of Isosorbide Dinitrate. Chemical and Pharmaceutical Bulletin, 38(3), 740–743. https://doi.org/10.1248/cpb.38.740

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