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大肠杆菌α-溶血素的钙结合C末端结构域是该蛋白质表面活性特性的主要决定因素。

The calcium-binding C-terminal domain of Escherichia coli alpha-hemolysin is a major determinant in the surface-active properties of the protein.

作者信息

Sánchez-Magraner Lissete, Viguera Ana R, García-Pacios Marcos, Garcillán M Pilar, Arrondo José-Luis R, de la Cruz Fernando, Goñi Félix M, Ostolaza Helena

机构信息

Unidad de Biofísica (Centro Mixto CSIC-UPV/EHU), Universidad del País Vasco, Aptdo. 644, 48080 Bilbao, Spain.

出版信息

J Biol Chem. 2007 Apr 20;282(16):11827-35. doi: 10.1074/jbc.M700547200. Epub 2007 Feb 26.

DOI:10.1074/jbc.M700547200
PMID:17324923
Abstract

alpha-Hemolysin (HlyA) from Escherichia coli is a protein toxin (1024 amino acids) that targets eukaryotic cell membranes, causing loss of the permeability barrier. HlyA consists of two main regions, an N-terminal domain rich in amphipathic helices, and a C-terminal Ca(2+)-binding domain containing a Gly- and Asp-rich nonapeptide repeated in tandem 11-17 times. The latter is called the RTX domain and gives its name to the RTX protein family. It had been commonly assumed that membrane interaction occurred mainly if not exclusively through the amphipathic helix domain. However, we have cloned and expressed the C-terminal region of HlyA, containing the RTX domain plus a few stabilizing sequences, and found that it is a potent surface-active molecule. The isolated domain binds Ca(2+) with about the same affinity (apparent K(0.5) approximately 150 microM) as the parent protein HlyA, and Ca(2+) binding induces in turn a more compact folding with an increased proportion of beta-sheet structure. Both with and without Ca(2+) the C-terminal region of HlyA can interact with lipid monolayers spread at an air-water interface. However, the C-terminal domain by itself is devoid of membrane lytic properties. The present results can be interpreted in the light of our previous studies that involved in receptor binding a peptide in the C-terminal region of HlyA. We had also shown experimentally the distinction between reversible membrane adsorption and irreversible lytic insertion of the toxin. In this context, the present data allow us to propose that both major domains of HlyA are directly involved in membrane-toxin interaction, the nonapeptide repeat, calcium-binding RTX domain being responsible for the early stages of HlyA docking to the target membrane.

摘要

来自大肠杆菌的α-溶血素(HlyA)是一种蛋白质毒素(1024个氨基酸),作用于真核细胞膜,导致通透性屏障丧失。HlyA由两个主要区域组成,一个富含两亲性螺旋的N端结构域,以及一个C端钙结合结构域,该结构域含有一个富含甘氨酸和天冬氨酸的九肽,串联重复11 - 17次。后者被称为RTX结构域,也是RTX蛋白家族名称的由来。通常认为膜相互作用主要(如果不是唯一)通过两亲性螺旋结构域发生。然而,我们克隆并表达了HlyA的C端区域,该区域包含RTX结构域以及一些稳定序列,发现它是一种有效的表面活性分子。分离出的结构域与钙离子结合的亲和力(表观K(0.5)约为150微摩尔)与亲本蛋白HlyA大致相同,钙离子结合反过来会诱导更紧密的折叠,β-折叠结构比例增加。无论有无钙离子,HlyA的C端区域都能与在气-水界面铺展的脂质单层相互作用。然而,C端结构域本身没有膜溶解特性。根据我们之前涉及HlyA C端区域肽与受体结合的研究,可以对目前的结果进行解释。我们还通过实验证明了毒素可逆膜吸附和不可逆溶解插入之间的区别。在此背景下,目前的数据使我们能够提出,HlyA的两个主要结构域都直接参与膜-毒素相互作用,富含九肽重复序列、可结合钙的RTX结构域负责HlyA与靶膜对接的早期阶段。

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