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Isostatic compression, a new process for incorporating vancomycin into biphasic calcium phosphate: comparison with a classical method.

作者信息

Gautier H, Merle C, Auget J L, Daculsi G

机构信息

Laboratoire de Pharmacie Galénique, Centre de Recherche sur les Matériaux d'intérêt Biologique, UPRES EA 2159, Equipe INSERM 99-03, France.

出版信息

Biomaterials. 2000 Feb;21(3):243-9. doi: 10.1016/s0142-9612(99)00139-8.

DOI:10.1016/s0142-9612(99)00139-8
PMID:10646940
Abstract

Isostatic compression has rarely been used to load calcium-phosphate biomaterials with therapeutic agents. This report, concerning four processes associating vancomycin, compares isostatic compression with wet granulation, a classical method. In the wet granulation study, vancomycin was associated with biphasic calcium-phosphate (BCP) granules either by adsorption or incorporation with a new granulation. In the isostatic compression study, BCP powder was compressed at 100, 140 and 200 MPa. The blocks obtained were crushed and 200-500 microm, sieved; thus, the vancomycin solution was absorbed on these granules. Compaction of BCP and vancomycin powders gave, after crushing and sieving, granules loaded with vancomycin. In each study, 5% vancomycin was associated with BCP. Vancomycin release profiles were assessed by an in vitro culture chamber dissolution test. Physicochemical studies of BCP and vancomycin showed their structural integrity after isostatic compression. Isostatic compression prolonged vancomycin release time from 3 to 7 days and the release time became greater as isostatic pressure increased, probably because of the porosity decrease of the granules during compression.

摘要

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