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Functionalization of thioctic acid-capped gold nanoparticles for specific immobilization of histidine-tagged proteins

机译:硫辛酸封端的金纳米颗粒的功能化,用于组氨酸标签蛋白的特异性固定

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摘要

This paper presents an efficient strategy for the specific immobilization of fully functional proteins onto the surface of nanoparticles. Thioctic acid-derivatized gold clusters are used as a scaffold for further stepwise modification, leading to a cobalt(II)-terminated ligand shell. A histidine tag introduced by genetic engineering into a protein is coordinated to this transition metal ion. The specific immobilization has been demonstrated for the cases of a genetically engineered horseradish peroxidase and ferredoxin-NADP+ reductase, confirming the attachment of the fully functional proteins to the Co(II)-terminated nanointerface. The absence of nonspecific protein adsorption and the specificity of the binding site have been verified using several analogues of the enzymes without the histidine tag.
机译:本文提出了一种将全功能蛋白特异性固定在纳米颗粒表面的有效策略。硫辛酸衍生的金簇被用作进一步逐步修饰的支架,从而形成了以钴(II)为末端的配体壳。通过基因工程引入蛋白质的组氨酸标签与该过渡金属离子配位。对于基因工程辣根过氧化物酶和铁氧还蛋白-NADP +还原酶的情况,已经证明了特定的固定化作用,从而证实了功能齐全的蛋白质与Co(II)终止的纳米界面的结合。使用几种没有组氨酸标签的酶类似物已经证实了非特异性蛋白质的吸附和结合位点的特异性。

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