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葡萄球菌α-毒素形成通道需要部分C末端展开。

Partial C-terminal unfolding is required for channel formation by staphylococcal alpha-toxin.

作者信息

Vécsey-Semjén B, Möllby R, van der Goot F G

机构信息

Département de Biochimie, Université de Genève, 30 quai E. Ansermet, 1211 Genève, Switzerland.

出版信息

J Biol Chem. 1996 Apr 12;271(15):8655-60. doi: 10.1074/jbc.271.15.8655.

Abstract

The pore-forming alpha-toxin from Staphylococcus aureus is secreted as a soluble monomeric protein. In order to form a transmembrane channel, the protein has to undergo oligomerization and membrane insertion. Previous studies have shown that channel formation is favored by acidic pH. We have analyzed the effect of pH on the kinetics of channel formation as well as on the conformation of the toxin. Using a variety of spectroscopic probes for protein structure, we have shown that alpha-toxin unfolded upon acidification and that the unfolding process occurred in at least three steps. The various steps could be selectively affected by modifying the salt concentration or the temperature. This unfolding was, however, only partial as the secondary structure remained native-like as witnessed by far UV CD measurements. The first unfolding step, corresponding to a region of the C-terminal half of the toxin, is of particular importance as it coincided with the exposure of hydrophobic patches on the surface of the protein as well as with the onset of channel formation. Our observations strongly suggest that transition of the C-terminal half of alpha-toxin to a molten globule-like state is required for channel formation.

摘要

金黄色葡萄球菌形成孔道的α毒素以可溶性单体蛋白的形式分泌。为了形成跨膜通道,该蛋白必须经历寡聚化和膜插入过程。先前的研究表明,酸性pH有利于通道的形成。我们分析了pH对通道形成动力学以及毒素构象的影响。使用多种用于蛋白质结构的光谱探针,我们发现α毒素在酸化时会发生去折叠,且去折叠过程至少分三步进行。通过改变盐浓度或温度,可以选择性地影响各个步骤。然而,这种去折叠只是部分的,因为远紫外圆二色性测量表明二级结构仍保持类似天然的状态。第一个去折叠步骤对应于毒素C端一半的区域,尤为重要,因为它与蛋白质表面疏水斑块的暴露以及通道形成的开始同时发生。我们的观察结果强烈表明,α毒素C端一半转变为类似熔球的状态是通道形成所必需的。

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