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双膦酸盐控制释放系统在骨植入物中的研制:制剂和工艺对体外释放的影响。

Development of bisphosphonates controlled delivery systems for bone implantation: influence of the formulation and process used on in vitro release.

机构信息

INSERM, U 791, Laboratoire d'ingénierie ostéo-articulaire et dentaire, LIOAD, Université de Nantes, 1 Place Alexis Ricordeau, 44042, Nantes, France.

出版信息

J Mater Sci Mater Med. 2010 May;21(5):1599-604. doi: 10.1007/s10856-010-4012-x. Epub 2010 Feb 23.

Abstract

The present study investigates the development of controlled drug delivery devices by association of bisphosphonates (BPs) with calcium-deficient apatite (CDA) to obtain a prolonged drug delivery. In a first part, we studied the microencapsulation of methylene bisphosphonic acid, our model of BPs, in biodegradable PLGA by the double emulsion (w/o/w) solvent evaporation/extraction process. Secondly, we associated BPs, either in a free form or microencapsulated, with calcium phosphate biomaterials. The association of free BPs with CDA was performed by isostatic compression at 80 MPa and we tested the interest of adding a binder, HPMC, in the formulation to reinforce the association. In parallel, microparticles were associated with calcium-deficient apatite, either by simple mixture or by isostatic compression. To compare the different formulations, in vitro dissolution studies were performed. All the formulations tested appear to be efficient to produce BPs loaded biomaterials able to deliver the drug slowly and at a constant rate. The slowest release rate (2.7% in 14 days) was obtained with the blend of microencapsulated BPs with CDA.

摘要

本研究通过将双膦酸盐 (BPs) 与缺钙磷灰石 (CDA) 结合来开发控释药物输送装置,以实现药物的持续释放。在第一部分中,我们通过双重乳液 (w/o/w) 溶剂蒸发/萃取法研究了将我们的 BPs 模型亚甲基双膦酸微囊化到可生物降解的 PLGA 中。其次,我们将游离 BPs 或微囊化 BPs 与磷酸钙生物材料结合。游离 BPs 与 CDA 的结合是通过在 80 MPa 下等静压压缩来实现的,我们测试了在配方中添加 binder(HPMC)来增强结合的效果。同时,通过简单混合或等静压压缩将微球与缺钙磷灰石结合。为了比较不同的配方,我们进行了体外溶解研究。所有测试的配方似乎都能有效地制备负载 BPs 的生物材料,这些材料能够缓慢且持续地释放药物。在 14 天内释放率最慢(2.7%)的是微囊化 BPs 与 CDA 的混合物。

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