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炭疽毒素保护性抗原的晶体结构

Crystal structure of the anthrax toxin protective antigen.

作者信息

Petosa C, Collier R J, Klimpel K R, Leppla S H, Liddington R C

机构信息

Biochemistry Department, University of Leicester, UK.

出版信息

Nature. 1997 Feb 27;385(6619):833-8. doi: 10.1038/385833a0.

Abstract

Protective antigen (PA) is the central component of the three-part protein toxin secreted by Bacillus anthracis, the organism responsible for anthrax. After proteolytic activation on the host cell surface, PA forms a membrane-inserting heptamer that translocates the toxic enzymes, oedema factor and lethal factor, into the cytosol. PA, which has a relative molecular mass of 83,000 (M(r) 83K), can also translocate heterologous proteins, and is being evaluated for use as a general protein delivery system. Here we report the crystal structure of monomeric PA at 2.1 A resolution and the water-soluble heptamer at 4.5 A resolution. The monomer is organized mainly into antiparallel beta-sheets and has four domains: an amino-terminal domain (domain 1) containing two calcium ions and the cleavage site for activating proteases; a heptamerization domain (domain 2) containing a large flexible loop implicated in membrane insertion; a small domain of unknown function (domain 3); and a carboxy-terminal receptor-binding domain (domain 4). Removal of a 20K amino-terminal fragment from domain 1 allows the assembly of the heptamer, a ring-shaped structure with a negatively charged lumen, and exposes a large hydrophobic surface for binding the toxic enzymes. We propose a model of pH-dependent membrane insertion involving the formation of a porin-like, membrane-spanning beta-barrel.

摘要

保护性抗原(PA)是炭疽芽孢杆菌分泌的三部分组成的蛋白质毒素的核心成分,炭疽芽孢杆菌是导致炭疽病的病原体。在宿主细胞表面进行蛋白水解激活后,PA形成一种插入膜的七聚体,将毒性酶水肿因子和致死因子转运到细胞质中。相对分子质量为83,000(M(r) 83K)的PA也可以转运异源蛋白,目前正在评估其作为通用蛋白质递送系统的用途。在此,我们报告了单体PA在2.1埃分辨率下的晶体结构以及水溶性七聚体在4.5埃分辨率下的晶体结构。单体主要由反平行β折叠组成,有四个结构域:一个氨基末端结构域(结构域1),含有两个钙离子和激活蛋白酶的切割位点;一个七聚化结构域(结构域2),含有一个与膜插入有关的大的柔性环;一个功能未知的小结构域(结构域3);以及一个羧基末端受体结合结构域(结构域4)。从结构域1去除一个20K的氨基末端片段可使七聚体组装,七聚体是一种具有带负电荷内腔的环形结构,并暴露出一个大的疏水表面用于结合毒性酶。我们提出了一种pH依赖性膜插入模型,涉及形成一种类似孔蛋白的跨膜β桶。

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