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Effect of particle size of calcium phosphate based bioceramic drug delivery carrier on the release kinetics of ciprofloxacin hydrochloride: an in vitro study

机译:磷酸钙基生物陶瓷给药载体的粒径对盐酸环丙沙​​星释放动力学的影响:体外研究

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Hydroxyapatite (HAP) is the constituent of calcium phosphate based bone cement and it is extensively used as a bone substitute and drug delivery vehicle in various biomedical applications. In the present study we investigated the release kinetics of ciprofloxacin loaded HAP and analyzed its ability to function as a targeted and sustained release drug carrier. Synthesis of HAP was carried out by combustion method using tartaric acid as a fuel and nitric acid as an oxidizer. Powder XRD and FTIR techniques were employed to characterize the phase purity of the drug carrier and to verify the chemical interaction between the drug and carrier. The synthesized powders were sieve separated to make two different drug carriers with different particle sizes and the surface topography of the pellets of the drug carrier was imaged by AFM. Surface area and porosity of the drug carrier was carried out using surface area analyzer. The in-vitro drug release kinetics was performed in simulated body fluid, at 37.3℃. The amount of ciprofloxacin released is measured using UV-visible spectroscopy following the characteristic λ_(max) of 278 nm. The release saturates around 450 h which indicates that it can be used as a targeted and sustained release carrier for bone infections.
机译:羟基磷灰石(HAP)是磷酸钙基骨水泥的组成部分,在各种生物医学应用中被广泛用作骨替代品和药物递送载体。在本研究中,我们研究了载有环丙沙星的HAP的释放动力学,并分析了其作为靶向和持续释放药物载体的功能。通过使用酒石酸作为燃料和硝酸作为氧化剂的燃烧方法进行HAP的合成。采用粉末XRD和FTIR技术表征药物载体的相纯度,并验证药物与载体之间的化学相互作用。将合成的粉末过筛分离以制备两种具有不同粒径的不同药物载体,并且通过AFM对药物载体小丸的表面形貌进行成像。使用表面积分析仪进行药物载体的表面积和孔隙率。在37.3℃的模拟体液中进行体外药物释放动力学。使用紫外可见光谱法,按照278 nm的特征λ_(max)测定环丙沙星的释放量。释放在450小时左右达到饱和,这表明它可用作骨感染的靶向和持续释放载体。

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