Vancomycin encapsulation in biodegradable poly(ε-caprolactone) microparticles for bone implantation.: Influence of the formulation process on size, drug loading, in vitro release and cytocompatibility
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作者:
Le Ray, AM
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INSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, FranceINSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, France
Le Ray, AM
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Chiffoleau, S
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INSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, FranceINSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, France
Chiffoleau, S
[1
]
Iooss, P
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INSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, FranceINSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, France
Iooss, P
[1
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Grimandi, G
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INSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, FranceINSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, France
Grimandi, G
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Gouyette, A
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INSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, FranceINSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, France
Gouyette, A
[1
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Daculsi, G
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INSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, FranceINSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, France
Daculsi, G
[1
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Merle, C
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INSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, FranceINSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, France
Merle, C
[1
]
机构:
[1] INSERM, Equipe 99 03, Ctr Rech Mat Interet Biol, Pharm Galen Lab, F-44042 Nantes, France
microparticles;
poly(epsilon-caprolactone);
vancomycin;
solvent evaporation process;
in vitro release;
cytocompatibility;
D O I:
10.1016/S0142-9612(02)00357-5
中图分类号:
R318 [生物医学工程];
学科分类号:
0831 ;
摘要:
Vancomycin encapsulation in biodegradable poly(epsilon-caprolactone) microparticles (200 mum mean diameter) was most efficient with a simple emulsion technique that dispersed 122.5 mg/g of polymer. Scanning electron micrographs showed smooth or pitted particles. Dissolution studies were correlated with microparticle morphology, indicating higher release with pitted particles when vancomycin was encapsulated in a dissolved state. The cytocompatibility of these poly(epsilon-caprolactone) microparticles was demonstrated by a direct contact cytotoxic assay. This material can be considered as an efficient drug delivery system for bone implantation. (C) 2002 Elsevier Science Ltd. All rights reserved.