生物共代谢动力学模型-《郑州大学学报(工学版)》

文章信息/Info

Keywords:: Co-metabolism; Transformation capacity; biotransformation; toxicity; Microbial decline

摘要:: 共代谢转化率与生长期生长基质的消耗以及在缺乏生长基质条件下生物量和/或能源物质的消耗有关.对比了早先提出的关于休眠细胞的三种共代谢动力学模型(1～3),得出三种模型在高浓度生长基质存在时具有的共同特征,并提出在生长基质存在条件下非生长基质转化的表达式,将该表达式与细胞生长表达式合并所构成的方程描述了另一个完整模型(4),它涵盖了模型1～3的特征并同时适用于休眠细胞和生长细胞的共代谢动力学研究.模型(4)描述了非生长基质的转化及生长基质和生物量的消耗,预测共代谢导致了生物维持生长所需物质和衰减速率的增加以及

Abstract:: Co-metabolic conversion rate is related to the consumption of growth substrate during the growth period and the consumption of biomass and/or energy substances in the absence of growth substrate. By comparing the three co-metabolic kinetic models (1~3) proposed earlier on dormant cells, the common characteristics of the three models in the presence of high concentrations of growth matrix are obtained, and the expression of non-growth matrix transformation in the presence of growth matrix is proposed, and the equation formed by combining this expression with cell growth expression describes another complete model (4), which covers the characteristics of model 1~3 and is applicable to the co-metabolic dynamics of dormant cells and growing cells. Model (4) describes the transformation of non-growth substrates and the consumption of growth substrates and biomass, predicting that co-metabolism leads to an increase in the amount of substances required for biological growth and the rate of decay as well