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首页> 外文期刊>Journal of Non-Crystalline Solids: A Journal Devoted to Oxide, Halide, Chalcogenide and Metallic Glasses, Amorphous Semiconductors, Non-Crystalline Films, Glass-Ceramics and Glassy Composites >Optimization of ciprofloxacin release kinetics of novel Nano-bioactive glasses: Effect of glass modifier content on drug loading and release mechanism
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Optimization of ciprofloxacin release kinetics of novel Nano-bioactive glasses: Effect of glass modifier content on drug loading and release mechanism

机译:新型纳米生物活性玻璃释放动力学的优化释放动力学:玻璃改性剂含量对药物载荷和释放机理的影响

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摘要

This work aimed to prepare novel nano-bioactive glass compositions, belonging to the SiO2-CaO system, for local ciprofloxacin administration. As a new approach, drug loading and its release kinetics of glass nanoparticles were optimized by increasing the modifier content at the expense of glass former. Four different Glass samples, of 3.2, 13.8, 24.2, and 34.5 mol% CaO content, were prepared (coded as CS1, CS2, CS3 and CS4, respectively). They were characterized by TEM, DSC, TGA and FTIR. The glass samples exhibited specific surface areas of 299.3, 140.5, 81.59, and 17.58 (m(2).g(-1)), respectively. A strong correlation was established between the modifier contents of the glass samples and drug loading or release doses. Modeling the drug release profiles of all glass samples confirmed that drug was released via a controlled diffusion mean. All glass samples induced hydroxyapatite layer onto their surfaces after immersion in simulated body fluid.
机译:这种作品旨在制备新的纳米生物活性玻璃组合物,属于SiO2-CaO系统,用于局部环丙沙星给药。 作为一种新的方法,通过以玻璃前的牺牲含量提高改性剂含量来优化玻璃纳米颗粒的药物载荷及其释放动力学。 制备四种不同的玻璃样品,3.2,13.8,24.2和34.5mol%CaO含量(分别编码为CS1,CS2,CS3和CS4)。 它们的特点是TEM,DSC,TGA和FTIR。 玻璃样品分别显示出299.3,140.5,81.59和17.58(M(2).g(-1))的比表面积。 在玻璃样品和药物载荷或释放剂量的改性剂含量之间建立了强烈的相关性。 建模所有玻璃样品的药物释放曲线证实,通过受控扩散释放药物。 浸入模拟体液后,所有玻璃样品将羟基磷灰石层诱导到它们的表面上。

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