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Imaging mass spectrometry for assessing temporal proteomics: Analysis of calprotectin in acinetobacter baumannii pulmonary infection

机译:影像质谱法评估时间蛋白质组学:鲍曼不动杆菌肺部感染中钙卫蛋白的分析

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Imaging MS is routinely used to show spatial localization of proteins within a tissue sample and can also be employed to study temporal protein dynamics. The antimicrobial S100 protein calprotectin, a heterodimer of subunits S100A8 and S100A9, is an abundant cytosolic component of neutrophils. Using imaging MS, calprotectin can be detected as a marker of the inflammatory response to bacterial challenge. In a murine model of Acinetobacter baumannii pneumonia, protein images of S100A8 and S100A9 collected at different time points throughout infection aid in visualization of the innate immune response to this pathogen. Calprotectin is detectable within 6 h of infection as immune cells respond to the invading pathogen. As the bacterial burden decreases, signals from the inflammatory proteins decrease. Calprotectin is no longer detectable 96-144 h post infection, correlating to a lack of detectable bacterial burden in lungs. These experiments provide a label-free, multiplexed approach to study host response to a bacterial threat and eventual clearance of the pathogen over time.
机译:成像MS通常用于显示组织样品中蛋白质的空间定位,也可以用于研究时间蛋白质动力学。抗菌素S100蛋白钙卫蛋白是S100A8和S100A9亚基的异二聚体,是嗜中性粒细胞的丰富胞质成分。使用成像MS,可以将钙卫蛋白检测为对细菌攻击的炎症反应的标志。在鲍曼不动杆菌肺炎的鼠模型中,在整个感染过程中的不同时间点收集的S100A8和S100A9的蛋白质图像有助于可视化对该病原体的先天免疫应答。钙卫蛋白可以在感染后6小时内检测到,因为免疫细胞对入侵的病原体有反应。随着细菌负担的减少,来自炎症蛋白的信号会减少。感染后96-144小时不再检测到钙卫蛋白,这与肺中缺乏可检测的细菌负担有关。这些实验提供了一种无标记的多重方法来研究宿主对细菌威胁的反应以及随着时间的推移最终清除病原体。

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