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通过疏水相互作用组装氧化石墨烯-酶缀合物。

Assembly of graphene oxide-enzyme conjugates through hydrophobic interaction.

机构信息

National Key Laboratory of Micro/Nano Fabrication Technology, Key Laboratory for Thin Film and Microfabrication of the Ministry of Education, Research Institute of Micro/Nano Science and Technology, Shanghai Jiao Tong University, Shanghai 200240, P. R. China.

出版信息

Small. 2012 Jan 9;8(1):154-9. doi: 10.1002/smll.201101695. Epub 2011 Oct 31.

Abstract

Biochemical and biomedical applications of graphene oxide (GO) critically rely on the interaction of biomolecules with it. It has been previously reported that the biological activity of the GO-enzyme conjugate decreases due to electrostatic interaction between the enzymes and GO. Herein, the immobilization of horseradish peroxidase (HRP) and oxalate oxidase (OxOx) on chemically reduced graphene oxide (CRGO) are reported. The enzymes can be adsorbed onto CRGO directly with a tenfold higher enzyme loading than that on GO, and maximum enzyme loadings reach 1.3 and 12 mg mg(-1) for HRP and OxOx, respectively. Significantly, the more CRGO is reduced, the higher the enzyme loading. The CRGO-HRP conjugates also exhibit higher enzyme activity and stability than GO-HRP. Excellent properties of the CRGO-enzyme conjugates are attributed to hydrophobic interaction between the enzymes and the CRGO. The hydrophobic interaction mode of the CRGO-enzyme conjugates can be applied to other hydrophobic proteins, and thus could dramatically improve the performance of immobilized proteins. The results indicate that CRGO is a potential substrate for efficient enzyme immobilization, and is an ideal candidate as a macromolecule carrier and biosensor.

摘要

氧化石墨烯(GO)的生物化学和生物医学应用严重依赖于生物分子与其的相互作用。先前已有报道称,由于酶与 GO 之间的静电相互作用,GO-酶缀合物的生物活性降低。在此,报道了辣根过氧化物酶(HRP)和草酸盐氧化酶(OxOx)在化学还原氧化石墨烯(CRGO)上的固定化。酶可以直接吸附在 CRGO 上,其酶负载量比在 GO 上高十倍,HRP 和 OxOx 的最大酶负载量分别达到 1.3 和 12 mg mg(-1)。重要的是,CRGO 被还原的越多,酶的负载量越高。CRGO-HRP 缀合物也表现出比 GO-HRP 更高的酶活性和稳定性。CRGO-酶缀合物的优异性能归因于酶与 CRGO 之间的疏水相互作用。CRGO-酶缀合物的疏水相互作用模式可应用于其他疏水蛋白,从而可显著改善固定化蛋白的性能。结果表明,CRGO 是一种有效的酶固定化的潜在基质,是一种理想的大分子载体和生物传感器候选材料。

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