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Gold nanoparticle-based tool to study protein conformational variants:implications in hemoglobinopathy

机译:基于金纳米粒子的工具,用于研究蛋白质构象变异:对血红蛋白病的意义

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The size of gold nanoparticles is shown here to gradually decrease if it is allowed to grow on a protein template,and the protein is subjected to unfolding by a nonionic denaturant.The correlation between size of the gold nanoparticle formed and the plasmon frequency observed remains linear,except at stages where protein folding intermediates are formed.Higher population of exposed tyrosine residues,number of sulfhydryl groups of the protein,and the overall exposition of the inner hydrophobic core may lead to the generation of smaller particles.The method provides a simple colorimetric sensing of protein conformation and has been tested for both nonheme and heme proteins (hemoglobin and bovine serum albumin).Similarly,protein variants with defects in folding (caused by subunit misassembly or mutation) can also be classified.Possible application of this approach in hemoglobinopathy (e.g.,thalassemia carrier detection) is discussed in the text.
机译:如果允许其在蛋白质模板上生长,金纳米颗粒的尺寸会逐渐减小,并且蛋白质会通过非离子变性剂展开。除形成蛋白质折叠中间体的阶段外。大量暴露的酪氨酸残基,蛋白质的巯基数量以及内部疏水核的整体暴露都可能导致产生较小的颗粒。该方法提供了一种简单的比色法蛋白质构象的检测,并已针对非血红素和血红素蛋白质(血红蛋白和牛血清白蛋白)进行了测试。同样,也可以对折叠缺陷的蛋白质变体(由亚基错配或突变引起)进行分类。这种方法在血红蛋白病中的可能应用(例如地中海贫血携带者检测)在本文中讨论。

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