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Cyclodextrin-responsive nanogel as an artificial chaperone for horseradish peroxidase

机译:环糊精响应纳米凝胶作为辣根过氧化物酶的人工伴侣

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摘要

The thermal stabilization and refolding of horseradish peroxidase (HRP) upon heating were investigated using an artificial molecular chaperone consisting of cholesterol-bearing pullulan (CHP) nanogels. The CHP nanogels inhibited the aggregation of HRP under heating by complexation with the denatured HRP. The enzyme activity of HRP complexed with CHP nanogels was not detected. However, the enzyme activity recovered up to 80% of native HRP after the addition of cyclodextrin (CD) to the complex. The dissociation of CHP nanogels was induced by the formation of an inclusion complex of cholesterol groups of CHP with CD. The enzyme activity of HRP was only significantly recovered by the addition of β-CD or its derivatives. Natural molecular chaperones, such as GroEL/ES, trap, fold, and release the nonnative proteins by changing the hydrophobicity of the specific sites of the molecular chaperone that interact with the nonnative protein. The functional mechanism of the nanogel chaperon system is similar to that of natural molecular chaperones. The nanogel chaperone system is a useful tool to aid the refolding and thermal stabilization of unstable proteins for post-genome research, and in medical and biological applications.
机译:使用由含胆固醇支链淀粉(CHP)纳米凝胶组成的人工分子伴侣,研究了辣根过氧化物酶(HRP)加热后的热稳定性和复性。 CHP纳米凝胶通过与变性的HRP络合,抑制了加热下HRP的聚集。未检测到HRP与CHP纳米凝胶复合的酶活性。但是,向复合物中添加环糊精(CD)后,酶的活性最多可恢复天然HRP的80%。 CHP纳米凝胶的解离是由CHP胆固醇基团与CD形成的包合物形成的。 HRP的酶活性仅通过添加β-CD或其衍生物才能显着恢复。诸如GroEL / ES的天然分子伴侣可以通过改变与伴侣蛋白相互作用的分子伴侣特定位点的疏水性来捕获,折叠和释放该伴侣蛋白。纳米凝胶分子伴侣系统的功能机理与天然分子伴侣分子相似。纳米凝胶分子伴侣系统是有用的工具,可帮助不稳定基因的重新折叠和热稳定化,以用于基因组后研究以及医学和生物学应用。

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