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Risk Assessment of Listeria monocytogenes: Impact of Individual Cell Variability on the Exposure Assessment Step

机译:单核细胞增生性李斯特菌的风险评估:个体细胞变异性对暴露评估步骤的影响

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摘要

Recently, the lag phase research in predictive microbiology is focusing more on the individual cell variability, especially for pathogenic microorganisms that typically occur in very low contamination levels, like Listeria monocytogenes. In this study, the effect of this individual cell lag phase variability was introduced in an exposure assessment study for L. monocytogenes in a liver pate. A basic framework was designed to estimate the contamination level of pate at the time of consumption, taking into account the frequency of contamination and the initial contamination levels of pate at retail. Growth was calculated on pate units of 150 g, comparing an individual-based approach with a classical population-based approach. The two different protocols were compared using simulations. If only the individual cell lag variability was taken into account, important differences were observed in cell density at the time of consumption between the individual-based approach and the classical approach, especially at low inoculum levels, resulting in high variability when using the individual-based approach. Although, when all variable factors were taken into account, no significant differences were observed between the different approaches, allowing the conclusion that the individual cell lag phase variability was overruled by the global variability of the exposure assessment framework. Even in more extreme conditions like a low inoculum level or a low water activity, no differences were created in cell density at the time of consumption between the individual-based approach and the classical approach. This means that the individual cell lag phase variability of L. monocytogenes has important consequences when studying specific growth cases, especially when the applied inoculum levels are low, but when performing more general exposure assessment studies, the variability between the individual cell lag phases is too limited to have a major impact on the total exposure assessment.
机译:最近,预测微生物学的滞后阶段研究更多地集中在单个细胞的变异性上,尤其是对于通常以极低污染水平出现的病原微生物,如单核细胞增生李斯特菌。在这项研究中,这种单个细胞滞后阶段变异性的影响被引入肝癌中单核细胞增生李斯特菌的暴露评估研究中。设计了一个基本框架来估计食用时果肉的污染水平,同时考虑了污染的频率和零售时果肉的初始污染水平。以150 g的脑袋单位计算生长量,将基于个体的方法与基于经典种群的方法进行了比较。使用仿真比较了两种不同的协议。如果仅考虑单个细胞滞后变异性,则基于个体的方法与经典方法之间在食用时的细胞密度会观察到重要差异,尤其是在低接种量时,导致使用单个个体的方法具有较高的变异性。基于方法。虽然,当考虑所有可变因素时,在不同方法之间未观察到显着差异,从而得出结论,暴露评估框架的整体可变性否定了单个细胞滞后阶段的可变性。即使在更极端的条件下,例如低接种量或低水分活度,基于个体的方法和传统方法之间在食用时细胞密度也不会产生差异。这意味着在研究特定生长病例时,单核细胞增生李斯特菌的单个细胞滞后阶段变异性具有重要的后果,特别是当所用接种物水平较低时,但是当进行更广泛的暴露评估研究时,单个细胞滞后阶段之间的变异性也很大。限制对总暴露评估有重大影响。

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