A proteomic approach for the identification of bismuth-binding proteins in Helicobacter pylori

被引:0
|
作者
Ruiguang Ge
Xuesong Sun
Qing Gu
Rory M. Watt
Julian A. Tanner
Benjamin Chun Yu Wong
Harry Huaxiang Xia
Jian-Dong Huang
Qing-Yu He
Hongzhe Sun
机构
[1] The University of Hong Kong,Department of Chemistry and Open Laboratory of Chemical Biology
[2] The University of Hong Kong,Department of Biochemistry, Li Ka Shing Faculty of Medicine
[3] The University of Hong Kong,Department of Medicine, Li Ka Shing Faculty of Medicine
[4] Jinan University,Institute of Life and Health Engineering
来源
JBIC Journal of Biological Inorganic Chemistry | 2007年 / 12卷
关键词
Colloidal bismuth subcitrate; Immobilized-metal affinity chromatography; Proteomics; Reactive oxygen species;
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学科分类号
摘要
Helicobacter pylori is a major human pathogen that can cause peptic ulcers and chronic gastritis. Bismuth-based triple or quadruple therapies are commonly recommended for the treatment of H. pylori infections. However, the molecular mechanisms underlying treatment with bismuth are currently not fully understood. We have conducted a detailed comparative proteomic analysis of H. pylori cells both before and after treatment with colloidal bismuth subcitrate (CBS). Eight proteins were found to be significantly upregulated or downregulated in the presence of CBS (20 μg mL−1). Bismuth-induced oxidative stress was confirmed by detecting higher levels of lipid hydroperoxide (approximately 1.8 times) and hemin (approximately 3.4 times), in whole cell extracts of bismuth-treated H. pylori cells, compared with those from untreated cells. The presence of bismuth also led to an approximately eightfold decrease in cellular protease activities. Using immobilized-bismuth affinity chromatography, we isolated and subsequently identified seven bismuth-binding proteins from H. pylori cell extracts. The intracellular levels of four of these proteins (HspA, HspB, NapA and TsaA) were influenced by the addition of CBS, which strongly suggests that they interact directly with bismuth. The other bismuth-interacting proteins identified were two enzymes (fumarase and the urease subunit UreB), and a translational factor (Ef-Tu). Our data suggest that the inhibition of proteases, modulation of cellular oxidative stress and interference with nickel homeostasis may be key processes underlying the molecular mechanism of bismuth’s actions against H. pylori.
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页码:831 / 842
页数:11
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