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A global Staphylococcus aureus proteome resource applied to the in vivo characterization of host-pathogen interactions

机译:全球金黄色葡萄球菌蛋白质组资源应用于宿主-病原体相互作用的体内表征

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摘要

Data-independent acquisition mass spectrometry promises higher performance in terms of quantification and reproducibility compared to data-dependent acquisition mass spectrometry methods. To enable high-accuracy quantification of Staphylococcus aureus proteins, we have developed a global ion library for data-independent acquisition approaches employing high-resolution time of flight or Orbitrap instruments for this human pathogen. We applied this ion library resource to investigate the time-resolved adaptation of S. aureus to the intracellular niche in human bronchial epithelial cells and in a murine pneumonia model. In epithelial cells, abundance changes for more than 400 S. aureus proteins were quantified, revealing, e.g., the precise temporal regulation of the SigB-dependent stress response and differential regulation of translation, fermentation, and amino acid biosynthesis. Using an in vivo murine pneumonia model, our data-independent acquisition quantification analysis revealed for the first time the in vivo proteome adaptation of S. aureus. From approximately 2.15 × 105  S. aureus cells, 578 proteins were identified. Increased abundance of proteins required for oxidative stress response, amino acid biosynthesis, and fermentation together with decreased abundance of ribosomal proteins and nucleotide reductase NrdEF was observed in post-infection samples compared to the pre-infection state.
机译:与数据无关的采集质谱方法相比,与数据无关的采集质谱法在定量和重现性方面具有更高的性能。为了能够对金黄色葡萄球菌蛋白进行高精度定量,我们已经开发了一种全球离子库,用于使用这种人类病原体的高分辨率飞行时间或Orbitrap仪器的数据独立采集方法。我们应用此离子库资源来调查时间分辨的金黄色葡萄球菌对人支气管上皮细胞和小鼠肺炎模型中细胞内生态位的适应性。在上皮细胞中,定量分析了400多种金黄色葡萄球菌蛋白质的丰度变化,从而揭示了SigB依赖性应激反应的精确时间调控以及翻译,发酵和氨基酸生物合成的差异调控。使用体内鼠类肺炎模型,我们独立于数据的采集定量分析首次揭示了金黄色葡萄球菌的体内蛋白质组适应性。从大约2.15××10 10 5的金黄色葡萄球菌细胞中,鉴定出578种蛋白质。与感染前相比,感染后样品中氧化应激反应,氨基酸生物合成和发酵所需的蛋白质丰度增加,而核糖体蛋白质和核苷酸还原酶NrdEF的丰度降低。

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