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Reaction–diffusion theory explains hypoxia and heterogeneous growth within microbial biofilms associated with chronic infections

机译:反应扩散理论解释了与慢性感染有关的微生物生物膜内的缺氧和异质生长

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摘要

Reaction–diffusion models were applied to gain insight into the aspects of biofilm infection and persistence by comparing mathematical simulations with the experimental data from varied bacterial biofilms. These comparisons, including three in vitro systems and two clinical investigations of specimens examined ex vivo, underscored the central importance of concentration gradients of metabolic substrates and the resulting physiological heterogeneity of the microorganisms. Relatively simple one-dimensional and two-dimensional (2D) models captured the: (1) experimentally determined distribution of specific growth rates measured in Pseudomonas aeruginosa cells within sputum from cystic fibrosis patients; (2) pattern of relative growth rate within aggregates of streptococcal biofilm harboured in an endocarditis vegetation; (3) incomplete penetration of oxygen into a Pseudomonas aeruginosa biofilm under conditions of exposure to ambient air and also pure oxygen; (4) localisation of anabolic activity around the periphery of P. aeruginosa cell clusters formed in a flow cell and attribution of this pattern to iron limitation; (5) very low specific growth rates, as small as 0.025 h−1, in the interior of cell clusters within a Klebsiella pneumoniae biofilm in a complex 2D domain of variable cell density.
机译:通过将数学模拟与来自各种细菌生物膜的实验数据进行比较,应用了反应扩散模型来深入了解生物膜感染和持久性方面。这些比较包括三个体外系统和两个离体检查标本的临床研究,强调了代谢底物浓度梯度和所产生微生物的生理异质性的重要性。相对简单的一维和二维(2D)模型捕获了:(1)实验确定的囊性纤维化患者痰中铜绿假单胞菌细胞中比生长速率的分布; (2)心内膜炎植被中所含链球菌生物膜聚集体中相对生长速率的模式; (3)在暴露于环境空气以及纯氧的条件下,氧气无法完全渗透到铜绿假单胞菌生物膜中; (4)在流通池中形成的铜绿假单胞菌细胞簇周围的合成代谢活性的定位,并将这种模式归因于铁限制; (5)在可变细胞密度的复杂二维域中,肺炎克雷伯菌生物膜内细胞簇内部的单位生长速率非常低,低至0.025 h -1

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