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首页> 外文期刊>Journal of mass spectrometry: JMS >Modeling bacteriophage amplification as a predictive tool for optimized MALDI-TOF MS-based bacterial detection
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Modeling bacteriophage amplification as a predictive tool for optimized MALDI-TOF MS-based bacterial detection

机译:将噬菌体扩增建模为优化基于MALDI-TOF MS的细菌检测的预测工具

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摘要

Matrix-assisted laser desorption/ionization time-of-flight mass spectrometry (MALDI-TOF MS) is a valuable tool for rapid bacterial detection and identification but is limited by the need for relatively high cell count samples, which have been grown under strictly controlled conditions. These requirements can be eliminated by the natural infection of a viable bacterial species of interest with a host-specific phage. This produces a rapid increase in phage protein concentrations in comparison to bacterial concentrations, which can in turn be exploited as a method for signal amplification during MALDI-TOF MS. One drawback to this approach is the requirement for repetitive, time-consuming sample preparation and analysis applied over the course of a phage infection to monitor phage concentrations as a function of time to determine the MALDI-TOF MS detection limit. To reduce the requirement for repeated preparation and analysis, a modified phage therapy model was investigated as a means for predicting the time during a given phage infection when a detectable signal would occur. The modified model used a series of three differential equations composed of predetermined experimental parameters including phage burst size and burst time to predict progeny phage concentrations as a function of time. Using Yersinia pestis with plague diagnostic phage φA1122 and Escherichia coli with phage MS2 as two separate, well-characterized model phage-host pairs, we conducted in silico modeling of the infection process and compared it with experimental infections monitored in real time by MALDI-TOF MS. Significant agreement between mathematically calculated phage growth curves and those experimentally obtained by MALDI-TOF MS was observed, thus verifying this method's utility for significant time and labor reduction.
机译:基质辅助激光解吸/电离飞行时间质谱(MALDI-TOF MS)是用于快速检测和鉴定细菌的有价值的工具,但受限于对细胞数量相对较高的样品的需求,这些样品必须在严格控制下生长条件。通过用宿主特异性噬菌体自然感染感兴趣的活细菌物种,可以消除这些要求。与细菌浓度相比,这会使噬菌体蛋白浓度迅速增加,这又可以用作MALDI-TOF MS期间信号放大的方法。这种方法的一个缺点是需要在噬菌体感染过程中进行重复,费时的样品制备和分析,以监测作为时间函数的噬菌体浓度,以确定MALDI-TOF MS检测限。为了减少重复制备和分析的需求,研究了一种改良的噬菌体治疗模型,作为预测在给定噬菌体感染期间会出现可检测信号的时间的手段。修改后的模型使用了一系列由预定的实验参数(包括噬菌体爆发大小和爆发时间)组成的三个微分方程来预测子代噬菌体浓度随时间的变化。使用鼠疫耶尔森氏菌和鼠疫诊断噬菌体φA1122和大肠杆菌和噬菌体MS2作为两个单独的,特征明确的模型噬菌体-宿主对,我们对感染过程进行了计算机模拟,并将其与通过MALDI-TOF实时监测的实验感染进行了比较多发性硬化症。观察到数学计算的噬菌体生长曲线与MALDI-TOF MS实验获得的曲线之间存在显着一致性,从而证明了该方法在节省大量时间和劳动力方面的效用。

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