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纳米羟基磷灰石微球作为抗生素递送系统:释放动力学、抗菌活性及其与成骨细胞的相互作用

Nanohydroxyapatite microspheres as delivery system for antibiotics: release kinetics, antimicrobial activity, and interaction with osteoblasts.

作者信息

Ferraz M P, Mateus A Y, Sousa J C, Monteiro F J

机构信息

INEB-Instituto de Engenharia Biomédica, Laboratório de Biomateriais, Rua do Campo Alegre, 823, 4150-180 Porto, Portugal.

出版信息

J Biomed Mater Res A. 2007 Jun 15;81(4):994-1004. doi: 10.1002/jbm.a.31151.

Abstract

Severe periodontitis treatment, where massive alveolar bone loss occurs, involves bone defect filling and intensive systemic log-term antibiotics administration. This study aims at developing novel injectable drug delivery systems (nanohydroxyapatite microspheres) with the drug releasing capability for periodontitis treatment and simultaneously initiating the osteointegration process. Materials were characterized by XRD, SEM, inverted stand optical microscope analysis, and mercury porosimetry method. Amoxicillin, amoxicillin + clavulanic acid, and erythromycin were the antibiotics used. Release properties during 28 days from the hydroxyapatite (HA) granules, and two types of nanoHA microspheres were investigated. Biocompatibility was assessed by cytotoxicity assays. HA granules were inadequate, releasing all antibiotic during the first hours. The concentration of antibiotics released in the first days from HA-2 was higher than from HA-1 microspheres, because of the increased porosity and surface area. The release profiles (fast initial release followed by long-term sustained release) of effective doses of antibiotics make these systems good alternatives for antibiotics delivery. Osteoblasts proliferated well on both types of microspheres, being cell growth enhanced in the presence of antibiotics. Erythromycin presented the most beneficial effect. Combining the sustained antibiotic release with the osteoconduction, resorbability, and potential use as injectable bone filling material of porous HA microspheres, these systems provided a forth fold beneficial effect.

摘要

重度牙周炎的治疗,若出现大量牙槽骨丧失,需进行骨缺损填充并长期大量使用全身性抗生素。本研究旨在开发具有药物释放能力的新型可注射给药系统(纳米羟基磷灰石微球)用于牙周炎治疗,并同时启动骨整合过程。通过X射线衍射(XRD)、扫描电子显微镜(SEM)、倒置光学显微镜分析和压汞法对材料进行表征。使用的抗生素为阿莫西林、阿莫西林+克拉维酸和红霉素。研究了羟基磷灰石(HA)颗粒以及两种类型的纳米HA微球在28天内的释放特性。通过细胞毒性试验评估生物相容性。HA颗粒效果不佳,在最初几小时内就释放了所有抗生素。由于孔隙率和表面积增加,HA-2微球在最初几天释放的抗生素浓度高于HA-1微球。有效剂量抗生素的释放曲线(初始快速释放随后长期持续释放)使这些系统成为抗生素递送的良好选择。成骨细胞在两种微球上均增殖良好,在有抗生素存在的情况下细胞生长增强。红霉素呈现出最有益的效果。将抗生素的持续释放与多孔HA微球的骨传导性、可吸收性以及作为可注射骨填充材料的潜在用途相结合,这些系统提供了四重有益效果。

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