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Temperature-responsive polymer-assisted protein refolding

机译:温度响应性聚合物辅助蛋白复性

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摘要

The mechanism of poly (N-isopropylacrylamide) (PNIPAAm)-assisted protein folding was investigated. An optimal concentration equivalent to a molar ratio of polymer to carbonic anhydrase B (CAB) of ca. 2 was observed, in which the refolding yield was improved by 28%. At concentration above the critical level, PNIPAAm promotes protein precipitation leading to lower refolding yields, which is more significant when high molecular weight polymers are used. Results of fluorescence analysis and equilibrium studies indicate that PNIPAAm enhances protein refolding by the formation of complexes with aggregation-prone folding intermediates via hydrophobic interactions, as PEG. Results of stepwise dilution experiments indicate the aggregation-prone intermediates of CAB populate at guanidine hydrochloride (GdnHCl) ranging from 2 to 1 M, which are stabilized by the chaotropic agent and may rapidly associate rapidly into insoluble aggregates upon further dilution via hydrophobic interactions. It was also shown that the formation of about one-third of the aggregates was mediated by unidentified processes other than the self-association of the aggregation-prone intermediates.
机译:研究了聚(N-异丙基丙烯酰胺)(PNIPAAm)辅助蛋白质折叠的机理。最佳浓度相当于聚合物与碳酸酐酶B(CAB)的摩尔比约观察到2,其中重折叠产率提高了28%。在高于临界水平的浓度下,PNIPAAm会促进蛋白质沉淀,导致较低的重折叠产量,这在使用高分子量聚合物时更为明显。荧光分析和平衡研究的结果表明,PNIPAAm通过与具有聚集倾向的折叠中间体通过疏水相互作用形成复合物(如PEG)来增强蛋白质的折叠。逐步稀释实验的结果表明,CAB的易于聚集的中间体在2到1 M的盐酸胍(GdnHCl)处形成,并由离液剂稳定,在通过疏水作用进一步稀释后可迅速缔合成不溶的聚集体。还表明,聚集体的约三分之一的形成是由除聚集倾向的中间体的自缔合以外的未确定的过程所介导的。

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