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GroE协助重组人尿激酶原的重折叠。

GroE assists refolding of recombinant human pro-urokinase.

作者信息

Xu Z, Yang S, Zhu D

机构信息

Department of Biochemistry, Nanjing University, China.

出版信息

J Biochem. 1997 Feb;121(2):331-7. doi: 10.1093/oxfordjournals.jbchem.a021591.

Abstract

GroE, one of the molecular chaperones, facilitates correct protein folding both in vitro and in vivo. The refolding of recombinant human pro-urokinase, a protein with a high content of disulfide bonds, was used as a model system to illustrate the mechanism of action of GroE. Aggregation of this protein predominates during its in vitro refolding, as indicated by a strong, concentration-dependent increase in light scattering. The addition of GroE and Mg-ATP significantly increases the yield of the active protein. GroE specifically inhibits the aggregation reaction that competes with correct folding, as shown by a strong decrease in the intensity of light scattering. GroEL rapidly binds to unfolded or partially folded pro-urokinase molecules and thus protects them from the aggregation reaction. Interaction with GroES and ATP hydrolysis are required for the release of the polypeptide chain from GroEL and further acquisition of the completely folded, native conformation.

摘要

分子伴侣之一的GroE在体外和体内都有助于蛋白质正确折叠。重组人尿激酶原是一种含有高含量二硫键的蛋白质,其重折叠被用作模型系统来说明GroE的作用机制。如光散射强烈且浓度依赖性增加所示,该蛋白质在体外重折叠过程中主要发生聚集。添加GroE和Mg-ATP可显著提高活性蛋白的产量。如光散射强度大幅降低所示,GroE特异性抑制与正确折叠竞争的聚集反应。GroEL迅速结合未折叠或部分折叠的尿激酶原分子,从而保护它们不发生聚集反应。从GroEL释放多肽链并进一步获得完全折叠的天然构象需要与GroES相互作用和ATP水解。

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