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Dynamical Model of Drug Accumulation in Bacteria: Sensitivity Analysis and Experimentally Testable Predictions

机译:细菌中药物蓄积的动力学模型:敏感性分析和实验可预测的预测

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摘要

We present a dynamical model of drug accumulation in bacteria. The model captures key features in experimental time courses on ofloxacin accumulation: initial uptake; two-phase response; and long-term acclimation. In combination with experimental data, the model provides estimates of import and export rates in each phase, the time of entry into the second phase, and the decrease of internal drug during acclimation. Global sensitivity analysis, local sensitivity analysis, and Bayesian sensitivity analysis of the model provide information about the robustness of these estimates, and about the relative importance of different parameters in determining the features of the accumulation time courses in three different bacterial species: Escherichia coli, Staphylococcus aureus, and Pseudomonas aeruginosa. The results lead to experimentally testable predictions of the effects of membrane permeability, drug efflux and trapping (e.g., by DNA binding) on drug accumulation. A key prediction is that a sudden increase in ofloxacin accumulation in both E. coli and S. aureus is accompanied by a decrease in membrane permeability.
机译:我们提出了一种在细菌中积累药物的动力学模型。该模型捕捉了氧氟沙星积累的实验时间过程中的关键特征:初始摄入量;两相响应和长期适应。结合实验数据,该模型可以估算每个阶段的进出口率,进入第二阶段的时间以及适应过程中内部药物的减少。该模型的全局敏感性分析,局部敏感性分析和贝叶斯敏感性分析提供了有关这些估计值的稳健性以及不同参数在确定三种不同细菌物种中累积时间过程的特征方面的相对重要性的信息:金黄色葡萄球菌和铜绿假单胞菌。结果导致膜渗透性,药物流出和捕获(例如,通过DNA结合)对药物积累的影响的实验可测试的预测。一个关键的预测是氧氟沙星在大肠杆菌和金黄色葡萄球菌中积累的突然增加伴随着膜通透性的降低。

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