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首页> 外文期刊>International Journal of Pharmaceutics >Modulation of Alendronate release from a calcium phosphate bone cement: An in vitro osteoblast-osteoclast co-culture study
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Modulation of Alendronate release from a calcium phosphate bone cement: An in vitro osteoblast-osteoclast co-culture study

机译:从磷酸钙骨水泥中的醛膦酸释放的调节:体外骨赘 - 破骨细胞共培养研究

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摘要

In this study, we loaded a biomimetic calcium phosphate bone cement (CPC) with relatively high amounts of a bisphosphonate through the use of Solid Lipid Microparticles (MPs) and investigated bone cells response to the composite cements. 10, 20 and 30% w/w of Alendronate (AL) were successfully introduced into microparticles of Cutina HR and Precirol, which were prepared by means of spray-congealing technique. Addition of AL-loaded MPs to the cement composition provoked a lengthening of the setting and of the hardening processes. However, setting times were still in a range useful for clinical applications, except for the cements at the highest Alendronate content. The composite cements displayed a sustained drug release over time. Cements with the best performances in terms of setting, hardening, mechanical properties and drug release were submitted to in vitro tests using a co-culture model of osteoblast and osteoclast. The results showed that the use of MPs to enrich the cement composition with Alendronate provides materials able to inhibit osteoclast viability and activity, while promoting osteoblast viability and earlier differentiation, indicating that the MPs-cements are good delivery systems for bisphosphonates.
机译:在这项研究中,通过使用固体脂质微粒(MPS)并研究对复合水泥的抗骨细胞,将磷酸钙骨水泥(CPC)用相对大量的双膦酸盐加载了相对大量的双膦酸盐。成功地将10,20和30%w / w成功地引入Cutina HR和前导的微粒中,通过喷射夹持技术制备。向水泥组合物中加入Al负载的MPS引发了延长的设置和硬化过程。然而,除了最高的Alendronate含量的水泥之外,设定时间仍然是对临床应用的范围。随着时间的推移,复合水泥显示出持续的药物释放。使用骨细胞和破骨细胞的共培养模型提交了在设定,硬化,机械性能和药物释放方面具有最佳表现的水泥,以体外测试。结果表明,使用MPS以与阿仑膦酸盐富集水泥组合物提供能够抑制破骨细胞活力和活性的材料,同时促进成骨细胞活力和早期的分化,表明MPS-PENCE是双膦酸盐的良好递送系统。

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