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首页> 外文期刊>Analytical chemistry >Assessment of Binding Affinity between Drugs and Human Serum Albumin Using Nanoporous Anodic Alumina Photonic Crystals
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Assessment of Binding Affinity between Drugs and Human Serum Albumin Using Nanoporous Anodic Alumina Photonic Crystals

机译:使用纳米多孔阳极氧化铝光子晶体评估药物与人血清白蛋白之间的结合亲和力

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In this study, we report an innovative approach aiming to assess the binding affinity between drug molecules and human serum albumin by combining nanoporous anodic alumina rugate filters (NAA-RFs) modified with human serum albumin (HSA) and reflectometric interference spectroscopy (RIfS). NAA-RFs are photonic crystal structures produced by sinusoidal pulse anodization of aluminum that present two characteristic optical parameters, the characteristic reflection peak (lambda(peak)), and the effective optical thickness of the film (OTeff), which can be readily used as sensing parameters. A design of experiments strategy and an ANOVA analysis are used to establish the effect of the anodization parameters (i.e., anodization period and anodization offset) on the sensitivity of HSA-modified NAA-RFs toward indomethacin, a model drug. To this end, two sensing parameters are used, that is, shifts in the characteristic reflection peak (Delta lambda(peak)) and changes in the effective optical thickness of the film (Delta OTeff). Subsequently, optimized NAA-RFs are used as sensing platforms to determine the binding affinity between a set of drugs (i.e., indomethacin, coumarin, sulfadymethoxine, warfarin, and salicylic acid) and HSA molecules. Our results verify that the combination of HSA-modified NAA-RFs with RIfS can be used as a portable, low-cost, and simple system for establishing the binding affinity between drugs and plasma proteins, which is a critical factor to develop efficient medicines for treating a broad range of diseases and medical conditions.
机译:在这项研究中,我们报告了一种创新方法,旨在通过结合用人血清白蛋白(HSA)修饰的纳米多孔阳极氧化铝皱纹滤光片(NAA-RFs)和反射光谱法(RIfS)来评估药物分子与人血清白蛋白之间的结合亲和力。 NAA-RF是铝的正弦脉冲阳极氧化产生的光子晶体结构,具有两个特征光学参数,即特征反射峰(λ(峰值))和薄膜的有效光学厚度(OTeff),可以方便地用作感应参数。使用实验策略设计和ANOVA分析来建立阳极氧化参数(即,阳极氧化周期和阳极氧化偏移量)对HSA修饰的NAA-RF对模型药物吲哚美辛的敏感性的影响。为此,使用了两个感测参数,即,特征反射峰的位移(Δlambda(peak))和膜的有效光学厚度的变化(ΔOTeff)。随后,将优化的NAA-RF用作传感平台,以确定一组药物(消炎痛,香豆素,磺胺二甲氧嘧啶,华法林和水杨酸)与HSA分子之间的结合亲和力。我们的研究结果证明,HSA修饰的NAA-RF与RIfS的组合可以用作建立药物与血浆蛋白之间结合亲和力的便携式,低成本和简单系统,这是开发高效药物的关键因素。治疗各种疾病和医疗状况。

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