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通过在A亚基中引入工程二硫键提高热稳定性的大肠杆菌不耐热肠毒素的晶体结构

Crystal structure of heat-labile enterotoxin from Escherichia coli with increased thermostability introduced by an engineered disulfide bond in the A subunit.

作者信息

van den Akker F, Feil I K, Roach C, Platas A A, Merritt E A, Hol W G

机构信息

Department of Biochemistry, University of Washington, Seattle 98195-7420, USA.

出版信息

Protein Sci. 1997 Dec;6(12):2644-9. doi: 10.1002/pro.5560061219.

Abstract

Cholera toxin (CT) produced by Vibrio cholerae and heat-labile enterotoxin (LT-I), produced by enterotoxigenic Escherichia coli, are AB5 heterohexamers with an ADP-ribosylating A subunit and a GM1 receptor binding B pentamer. These toxins are among the most potent mucosal adjuvants known and, hence, are of interest both for the development of anti-diarrheal vaccines against cholera or enterotoxigenic Escherichia coli diarrhea and also for vaccines in general. However, the A subunits of CT and LT-I are known to be relatively temperature sensitive. To improve the thermostability of LT-I an additional disulfide bond was introduced in the A1 subunit by means of the double mutation N40C and G166C. The crystal structure of this double mutant of LT-I has been determined to 2.0 A resolution. The protein structure of the N40C/G166C double mutant is very similar to the native structure except for a few local shifts near the new disulfide bond. The introduction of this additional disulfide bond increases the thermal stability of the A subunit of LT-I by 6 degrees C. The enhancement in thermostability could make this disulfide bond variant of LT-I of considerable interest for the design of enterotoxin-based vaccines.

摘要

霍乱弧菌产生的霍乱毒素(CT)和产肠毒素大肠杆菌产生的不耐热肠毒素(LT-I)是AB5杂六聚体,由一个具有ADP-核糖基化作用的A亚基和一个与GM1受体结合的B五聚体组成。这些毒素是已知最强效的黏膜佐剂之一,因此,对于开发针对霍乱或产肠毒素大肠杆菌腹泻的抗腹泻疫苗以及一般疫苗都具有重要意义。然而,已知CT和LT-I的A亚基对温度相对敏感。为提高LT-I的热稳定性,通过N40C和G166C双突变在A1亚基中引入了一个额外的二硫键。已确定该LT-I双突变体的晶体结构分辨率为2.0埃。除了新二硫键附近的一些局部位移外,N40C/G166C双突变体的蛋白质结构与天然结构非常相似。这个额外二硫键的引入使LT-I的A亚基热稳定性提高了6摄氏度。热稳定性的增强可能使这种LT-I的二硫键变体在基于肠毒素的疫苗设计中具有相当大的吸引力。

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