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功能映射的hrpZ 假单胞菌毒素揭示了位点负责蛋白质寡聚化、脂质相互作用和植物防御诱导。

Functional mapping of harpin HrpZ of Pseudomonas syringae reveals the sites responsible for protein oligomerization, lipid interactions and plant defence induction.

机构信息

General Microbiology, Department of Biological and Environmental Sciences, FI-00014 University of Helsinki, Helsinki, Finland.

出版信息

Mol Plant Pathol. 2011 Feb;12(2):151-66. doi: 10.1111/j.1364-3703.2010.00655.x. Epub 2010 Aug 17.

Abstract

Harpin HrpZ is one of the most abundant proteins secreted through the pathogenesis-associated type III secretion system of the plant pathogen Pseudomonas syringae. HrpZ shows membrane-binding and pore-forming activities in vitro, suggesting that it could be targeted to the host cell plasma membrane. We studied the native molecular forms of HrpZ and found that it forms dimers and higher order oligomers. Lipid binding by HrpZ was tested with 15 different membrane lipids, with HrpZ interacting only with phosphatidic acid. Pore formation by HrpZ in artificial lipid vesicles was found to be dependent on the presence of phosphatidic acid. In addition, HrpZ was able to form pores in vesicles prepared from Arabidopsis thaliana plasma membrane, providing evidence for the suggested target of HrpZ in the host. To map the functions associated with HrpZ, we constructed a comprehensive series of deletions in the hrpZ gene derived from P. syringae pv. phaseolicola, and studied the mutant proteins. We found that oligomerization is mainly mediated by a region near the C-terminus of the protein, and that the same region is also essential for membrane pore formation. Phosphatidic acid binding seems to be mediated by two regions separate in the primary structure. Tobacco, a nonhost plant, recognizes, as a defence elicitor, a 24-amino-acid HrpZ fragment which resides in the region indispensable for the oligomerization and pore formation functions of HrpZ.

摘要

Harpin HrpZ 是植物病原菌丁香假单胞菌的致病相关 III 型分泌系统分泌的最丰富的蛋白质之一。HrpZ 在体外具有膜结合和孔形成活性,表明它可能被靶向宿主细胞质膜。我们研究了 HrpZ 的天然分子形式,发现它形成二聚体和更高阶的寡聚物。用 15 种不同的膜脂测试了 HrpZ 的脂质结合,发现 HrpZ 仅与磷脂酸相互作用。发现 HrpZ 在人工脂质囊泡中形成孔取决于磷脂酸的存在。此外,HrpZ 能够在拟南芥质膜制备的囊泡中形成孔,为 HrpZ 在宿主中的预期靶标提供了证据。为了绘制与 HrpZ 相关的功能图谱,我们构建了源自丁香假单胞菌 pv. phaseolicola 的 hrpZ 基因的一系列全面缺失,并研究了突变蛋白。我们发现寡聚化主要由蛋白质 C 末端附近的区域介导,该区域对于膜孔形成也是必需的。磷脂酸结合似乎由一级结构中分开的两个区域介导。烟草作为非宿主植物,识别作为防御激发子的 24 个氨基酸的 HrpZ 片段,该片段位于 HrpZ 寡聚化和孔形成功能所必需的区域。

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