首页> 美国卫生研究院文献>Iranian Journal of Pharmaceutical Research : IJPR >In-vitro study of Ketoprofen Release from Synthesized Silica Aerogels (as Drug Carriers) and Evaluation of Mathematical Kinetic Release Models
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In-vitro study of Ketoprofen Release from Synthesized Silica Aerogels (as Drug Carriers) and Evaluation of Mathematical Kinetic Release Models

机译:合成二氧化硅气凝胶(作为药物载体)释放酮洛芬的体外研究和数学动力学释放模型的评估

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摘要

Silica aerogels are porous and extremely lightweight nano-materials that show interesting properties. These materials, because of biocompatibility, non-harmful to the body, and special physical characteristics such as large surface area and low density have great potential for use in a drug delivery system (DDS). The focus of this study is the evaluation of the effects of silica aerogels on improving the release rate of Ketoprofen as a relevant model drug of poorly soluble drugs in water. The in-vitro release rate of a conventional crystalline form of pure drug and three samples of drug loaded silica aerogels with different densities, 0.033, 0.080, and 0.24 g/cm3 were measured and investigated. The results show that all three samples of silica aerogels considerably increased (p < 0.05) the rate of drug release compared to its crystalline form. The silica aerogel sample with the lowest density (0.033 gr/cm3) has demonstrated the highest release rate of the drug (approximately five times faster than pure drug). Thus, silica aerogels could be acceptable carriers for poorly soluble drugs that require treatment with the fast release. Moreover, three release kinetic models were fitted with in-vitro drug release data and evaluated. The results indicate that the First-Order model is the best fit with the in-vitro Ketoprofen release data. Finally, in this article, a new kinetic release equation was obtained based on the first order model and release data, with applying the density of silica aerogel as an effective index parameter. This equation was proposed to describe Ketoprofen release rate in silica aerogels.
机译:二氧化硅气凝胶是多孔且极其轻巧的纳米材料,具有令人感兴趣的特性。这些材料由于具有生物相容性,对人体无害以及特殊的物理特性(例如大表面积和低密度),具有在药物输送系统(DDS)中使用的巨大潜力。这项研究的重点是评估二氧化硅气凝胶对提高酮洛芬作为难溶性药物在水中的相关模型药物的释放速率的作用。测量并研究了常规晶体形式的纯药物和三种不同载药量的二氧化硅气凝胶样品的体外释放速率,这些样品的密度分别为0.033、0.080和0.24 g / cm 3 。结果表明,与晶体形式相比,所有三个二氧化硅气凝胶样品均显着提高了药物释放速率(p <0.05)。具有最低密度(0.033 gr / cm 3 )的二氧化硅气凝胶样品显示出最高的药物释放速率(比纯药物快约五倍)。因此,对于需要快速释放治疗的难溶性药物,二氧化硅气凝胶可能是可接受的载体。此外,将三种释放动力学模型与体外药物释放数据进行拟合并进行了评估。结果表明,First-Order模型与体外酮洛芬释放数据最匹配。最后,在本文的基础上,以二氧化硅气凝胶的密度为有效指标,建立了基于一阶模型和释放数据的动力学释放方程。提出该方程式来描述酮洛芬在二氧化硅气凝胶中的释放速率。

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