Controlled release of proteins from poly(L-lactic acid) coated polyisobutylcyanoacrylate microcapsules

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[1] Park, Tae Gwan
[2] Alonso, Maria J.
[3] Langer, Robert
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Park, Tae Gwan | 1797年 / Publ by John Wiley & Sons Inc, New York, NY, United States卷 / 52期
关键词
Coated materials - Copolymers - Drying - Emulsification - Emulsions - Molecular weight - Polyacrylates - Proteins - Solutions - Surface active agents;
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摘要
Poly(L-lactic acid)-coated polyisobutylcyanoacrylate microcapsules containing protein molecules were prepared by a single-step procedure based on either a double-emulsion-solvent evaporation method or a spray-drying method. First, an aqueous protein solution was emulsified in an organic phase of methylene chloride containing a wall-forming monomer (isobutylcyanoacrylate), various kinds of poly(L-lactic acid), and a surfactant. An immediate polymerization process of isobutylcyanoacrylate takes place at the W/O interface upon contact with hydroxide ion in the aqueous phase, leading to the formation of a polyisobutylcyanoacrylate wall around the aqueous droplets. This W/O emulsion was reemulsified in an aqueous solution to promote the solvent removal and, consequently, the precipitation of poly(L-lactic acid) onto polyisobutylcyanoacrylate microcapsules or was spray-dried to directly deposit the poly(L-lactic acid) on the wall. Three proteins, bovine serum albumin, horseradish peroxidase, and tetanus toxoid, were encapsulated in these poly(L-lactic acid)-coated polyisobutylcyanoacrylate microcapsules, and then their release profiles were examined in vitro as a function of molecular weight of poly(L-lactic acid) and its copolymers with glycolic acid. These formulations exhibited a low `burst' effect at initial incubation stages and released the proteins for extended periods of time. Subcutaneous injections of the tetanus toxoid-loaded microparticles into rats showed that the time course of immunization (antibody titer) can be controlled by the type of polymer matrices used.
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