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Merits of sponge-like PLGA microspheres as long-acting injectables of hydrophobic drug

Title
Merits of sponge-like PLGA microspheres as long-acting injectables of hydrophobic drug
Authors
Kim S.Sah H.
Ewha Authors
사홍기
SCOPUS Author ID
사홍기scopus
Issue Date
2019
Journal Title
Journal of Biomaterials Science, Polymer Edition
ISSN
0920-5063JCR Link
Citation
Journal of Biomaterials Science, Polymer Edition vol. 30, no. 18, pp. 1725 - 1743
Keywords
microencapsulationmicrospherespoly-d,l-lactide-co-glycolidespongy morphology
Publisher
Taylor and Francis Inc.
Indexed
SCIE; SCOPUS WOS scopus
Document Type
Article
Abstract
Our study was initiated to challenge the preconception that nonporous PLGA microspheres with compact matrices should be used to develop long-acting depot injectables of hydrophobic drugs. A simple, new oil-in-water emulsion technique was utilized to produce porous PLGA microspheres with a sponge-like skeleton. Then, their applicability to developing sustained-release depots of hydrophobic drugs was explored in this study. As control, nonporous microspheres with a compact matrix were produced following a typical solvent evaporation process. Both microsphere manufacturing processes used non-halogenated isopropyl formate and progesterone as a dispersed solvent and a model hydrophobic drug, respectively. Various attempts were made to evaluate critical quality attributes of the porous microspheres and the nonporous ones. Surprisingly, the former displayed interesting features from the viewpoints of manufacturability and microsphere quality. For example, the spongy microspheres improved drug encapsulation efficiency and particle size uniformity, inhibited drug crystallization during microencapsulation, and minimized the residual solvent content in microspheres. Furthermore, the porous microspheres provided continual drug release kinetics without a lag time and much faster drug release than the non-porous microspheres did. In summary, the porous and sponge-like PLGA microspheres might find lucrative applications in developing sustained release dosage forms of hydrophobic drugs. © 2019, © 2019 Informa UK Limited, trading as Taylor & Francis Group.
DOI
10.1080/09205063.2019.1659712
Appears in Collections:
약학대학 > 약학과 > Journal papers
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