首页> 美国卫生研究院文献>other >Versatile Methodology for Glycosurfaces: Direct Ligation of Nonderivatized Reducing Saccharides to Poly(pentafluorophenyl acrylate) Grafted Surfaces via Hydrazide Conjugation
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Versatile Methodology for Glycosurfaces: Direct Ligation of Nonderivatized Reducing Saccharides to Poly(pentafluorophenyl acrylate) Grafted Surfaces via Hydrazide Conjugation

机译:糖表面的通用方法:非酰化还原糖通过酰肼偶联直接连接到聚五氟苯基丙烯酸酯接枝表面

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摘要

In this work, we report a convenient and versatile strategy for surface-grafted glycopolymer constructs with the goal of surface modification that controls the chemical presentation and grafting density of carbohydrate side chains. This approach employs a difunctional hydrazine linker, chemically modified to an active ester containing poly(pentafluorophenyl acrylate) grafted scaffold, to conjugate a variety of saccharides through the reducing end. The successive conjugation steps are carried out under mild conditions and yield high surface densities of sugars, as high as 4.8 mnol·cm−2, capable of multivalency, with an intact structure and retained bioactivity. We also demonstrate that this glycosylated surface can bind specific lectins according to the structure of its pendant carbohydrate. To demonstrate bioactivity, this surface platform is used to study the binding events of a human respiratory tract pathogen, Mycoplasma pneumoniae, on surfaces conjugated with sialylated sugars.
机译:在这项工作中,我们报告了一种表面嫁接的糖聚合物结构的便捷且通用的策略,其目标是通过表面修饰来控制碳水化合物侧链的化学成分和接枝密度。该方法采用了一种双官能的肼连接基,该连接基经过化学修饰成含有聚(五氟苯基丙烯酸丙烯酸酯)接枝支架的活性酯,可通过还原端缀合多种糖类。连续的缀合步骤在温和的条件下进行,产生的糖表面密度高,高达4.8 mnol·cm -2 ,具有多重价,结构完整且保留了生物活性。我们还证明了这种糖基化表面可以根据其侧链碳水化合物的结构结合特定的凝集素。为了证明其生物活性,该表面平台用于研究人呼吸道病原体肺炎支原体在与唾液酸化糖缀合的表面上的结合事件。

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