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用于整合生物加工的梭菌共培养物的基因组规模代谢建模。

Genome-scale metabolic modeling of a clostridial co-culture for consolidated bioprocessing.

机构信息

Department of Chemical Engineering and Applied Chemistry, University of Toronto, 200 College Street, Toronto, Ontario, Canada.

出版信息

Biotechnol J. 2010 Jul;5(7):726-38. doi: 10.1002/biot.201000159.

Abstract

An alternative consolidated bioprocessing approach is the use of a co-culture containing cellulolytic and solventogenic clostridia. It has been demonstrated that the rate of cellulose utilization in the co-culture of Clostridium acetobutylicum and Clostridium cellulolyticum is improved compared to the mono-culture of C. cellulolyticum, suggesting the presence of syntrophy between these two species. However, the metabolic interactions in the co-culture are not well understood. To understand the metabolic interactions in the co-culture, we developed a genome-scale metabolic model of C. cellulolyticum comprising of 431 genes, 621 reactions, and 603 metabolites. The C. cellulolyticum model can successfully predict the chemostat growth and byproduct secretion with cellulose as the substrate. However, a growth arrest phenomenon, which occurs in batch cultures of C. cellulolyticum at cellulose concentrations higher than 6.7 g/L, cannot be predicted by dynamic flux balance analysis due to the lack of understanding of the underlying mechanism. These genome-scale metabolic models of the pure cultures have also been integrated using a community modeling framework to develop a dynamic model of metabolic interactions in the co-culture. Co-culture simulations suggest that cellobiose inhibition cannot be the main factor that is responsible for improved cellulose utilization relative to mono-culture of C. cellulolyticum.

摘要

另一种整合生物加工方法是使用含有纤维素分解菌和溶剂生成梭菌的共培养物。已经证明,与纤维素分解梭菌的单培养物相比,在丙酮丁醇梭菌和纤维素分解梭菌的共培养物中纤维素的利用速率得到了提高,这表明这两个物种之间存在共生关系。然而,共培养物中的代谢相互作用还不是很清楚。为了了解共培养物中的代谢相互作用,我们开发了一个包含 431 个基因、621 个反应和 603 个代谢物的纤维素分解梭菌的基因组规模代谢模型。该纤维素分解梭菌模型可以成功预测以纤维素为底物的恒化器生长和副产物分泌。然而,由于缺乏对潜在机制的理解,动态通量平衡分析无法预测纤维素浓度高于 6.7 g/L 时纤维素分解梭菌分批培养中的生长停滞现象。由于缺乏对潜在机制的理解,动态通量平衡分析无法预测纤维素浓度高于 6.7 g/L 时纤维素分解梭菌分批培养中的生长停滞现象。这些纯培养物的基因组规模代谢模型也已经使用群落建模框架进行了整合,以开发共培养物中代谢相互作用的动态模型。共培养模拟表明,纤维二糖抑制不能是相对于纤维素分解梭菌单培养物提高纤维素利用率的主要因素。

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