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自固化生物活性玻璃骨水泥中吲哚美辛的体外和体内释放

The in vitro and in vivo indomethacin release from self-setting bioactive glass bone cement.

作者信息

Otsuka M, Nakahigashi Y, Matsuda Y, Kokubo T, Yoshihara S, Fujita H, Nakamura T

机构信息

Department of Pharmaceutical Technology, Kobe Pharmaceutical University, Japan.

出版信息

Biomed Mater Eng. 1997;7(5):291-302.

PMID:9457380
Abstract

The in vivo and in vitro drug release profiles from a self-setting bioactive CaO-SiO2-P2O5 glass bone cement containing indomethacin as a model drug were investigated. The cement containing 2% and 5% indomethacin (IMC) powder hardened within 5 min after mixing with ammonium phosphate buffer. After setting, in vitro drug release from drug-loaded cement pellets in a simulated body fluid (SBF) at pH 7.25 and 37 degrees C continued for two weeks. The hardened cement gradually formed low-crystallinity hydroxyapatite during the drug release test in SBF. An IMC-loaded cement device (2% and 5% drug) was implanted in the subcutaneous tissue on the back of rats. The in vivo IMC release from the cement increased and attained maximum levels (Cmax of 2% and 5% drug-loaded cements was 0.27 and 3.37 micrograms/ml, respectively) at Tmax, 3 and 0.5 d, respectively, upon subcutaneous (s.c.) administration in rats. This suggested that the s.c. administration of the cement provided IMC release for a much longer period than s.c. administration of the solution, and the plasma IMC concentration was dependent on the drug concentration in the cement. The plasma IMC concentration and the area under the curve from 2% and 5% IMC-loaded cements in rats were dependent on the concentration of IMC in the cements. The in vivo IMC concentration in plasma obtained by the deconvolution method was much lower than that delivered in SBF in vitro. Scanning electron microscopy and photomicrographs of cross sections showed that the bioactive bone cement had excellent biocompatibility with the surrounding soft tissues.

摘要

研究了一种以吲哚美辛为模型药物的自固化生物活性CaO-SiO2-P2O5玻璃骨水泥的体内和体外药物释放曲线。含有2%和5%吲哚美辛(IMC)粉末的骨水泥与磷酸铵缓冲液混合后在5分钟内硬化。固化后,载药骨水泥微丸在pH 7.25、37℃的模拟体液(SBF)中的体外药物释放持续了两周。在SBF中的药物释放试验过程中,硬化的骨水泥逐渐形成低结晶度的羟基磷灰石。将载有IMC的骨水泥装置(2%和5%药物)植入大鼠背部的皮下组织。在大鼠皮下给药后,骨水泥中IMC的体内释放增加,并分别在3天和0.5天达到最大水平(2%和5%载药骨水泥的Cmax分别为0.27和3.37微克/毫升)。这表明皮下注射骨水泥比皮下注射溶液提供IMC释放的时间长得多,并且血浆IMC浓度取决于骨水泥中的药物浓度。大鼠中2%和5%载有IMC的骨水泥的血浆IMC浓度和曲线下面积取决于骨水泥中IMC的浓度。通过去卷积法获得的血浆中体内IMC浓度远低于体外在SBF中递送的浓度。扫描电子显微镜和横截面显微照片显示,生物活性骨水泥与周围软组织具有优异的生物相容性。

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