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利用差异氧化蛋白质足迹法探究炭疽芽孢杆菌保护性抗原pH依赖性前孔到孔的转变

Probing the pH-dependent prepore to pore transition of Bacillus anthracis protective antigen with differential oxidative protein footprinting.

作者信息

Smedley James G, Sharp Joshua S, Kuhn Jeffrey F, Tomer Kenneth B

机构信息

Laboratory of Structural Biology, National Institute of Environmental Health Sciences, National Institutes of Health, Department of Health and Human Services, P.O. Box 12233, Research Triangle Park, North Carolina 27709, USA.

出版信息

Biochemistry. 2008 Oct 7;47(40):10694-704. doi: 10.1021/bi800533t. Epub 2008 Sep 12.

Abstract

The protective antigen (PA) component of the anthrax toxin (ATx) plays an essential role in the pathogenesis of the bioterrorism bacterium Bacillus anthracis. After oligomerization on the cell surface and docking of lethal factor and/or edema factor, PA is internalized and undergoes a conformational change when exposed to the low pH of the endosome to form a membrane-penetrating pore. While the structure of the PA prepore has been determined, precise structural information regarding the pore state remains lacking. Oxidative protein footprinting (OPF) can provide dynamic structural information about a protein complex through analysis of amino acid oxidation both before and after a conformational change. In this study, PA at pH 7.5 and 5.5 was exposed to hydroxyl radicals generated by ionizing radiation. Mass spectrometry was then used to both identify and quantitate the extent of oxidation of differentially modified residues. Several residues were found to be more readily oxidized at pH 7.5, most of which clustered toward the bottom plane of the prepore heptamer. Two amino acids had greater oxidation rates at pH 5.5, both found on the outer periphery of the prepore. When the OPF results were mapped to a current computational model of the pore, the accessibilities of some residues were consistent with their modeled positions in the pore (i.e., Y688 and V619/I620), while data for other residues (W346 and M350) appeared to conflict with the model. The results from this study illustrate the utility of OPF in generating empirical structural information for yet undetermined structures and offering opportunities for refinement for models thereof.

摘要

炭疽毒素(ATx)的保护性抗原(PA)成分在生物恐怖主义细菌炭疽芽孢杆菌的发病机制中起着至关重要的作用。在细胞表面寡聚化以及致死因子和/或水肿因子对接后,PA被内化,并在暴露于内体的低pH值时发生构象变化,形成一个穿透膜的孔。虽然PA前体孔的结构已经确定,但关于孔状态的精确结构信息仍然缺乏。氧化蛋白足迹法(OPF)可以通过分析构象变化前后氨基酸的氧化情况,提供有关蛋白质复合物的动态结构信息。在本研究中,将pH值为7.5和5.5的PA暴露于电离辐射产生的羟基自由基中。然后使用质谱法来鉴定和定量差异修饰残基的氧化程度。发现有几个残基在pH值为7.5时更容易被氧化,其中大多数聚集在前体孔七聚体的底部平面。有两个氨基酸在pH值为5.5时具有更高的氧化速率,均位于前体孔的外周。当将OPF结果映射到当前的孔计算模型时,一些残基的可及性与其在孔中的模拟位置一致(即Y688和V619/I620),而其他残基(W346和M350)的数据似乎与该模型相冲突。本研究结果说明了OPF在生成尚未确定结构的经验性结构信息以及为其模型优化提供机会方面的实用性。

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