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利用资源平衡分析评估酿酒酵母表型的蛋白质组分配。

Evaluating proteome allocation of Saccharomyces cerevisiae phenotypes with resource balance analysis.

机构信息

Department of Chemical Engineering, The Pennsylvania State University, University Park, PA, 16802, USA; DOE Center for Advanced Bioenergy and Bioproducts Innovation, The Pennsylvania State University, University Park, PA, 16802, USA.

Department of Chemical Engineering, The Pennsylvania State University, University Park, PA, 16802, USA; DOE Center for Advanced Bioenergy and Bioproducts Innovation, The Pennsylvania State University, University Park, PA, 16802, USA.

出版信息

Metab Eng. 2023 May;77:242-255. doi: 10.1016/j.ymben.2023.04.009. Epub 2023 Apr 18.

Abstract

Saccharomyces cerevisiae is an important model organism and a workhorse in bioproduction. Here, we reconstructed a compact and tractable genome-scale resource balance analysis (RBA) model (i.e., named scRBA) to analyze metabolic fluxes and proteome allocation in a computationally efficient manner. Resource capacity models such as scRBA provide the quantitative means to identify bottlenecks in biosynthetic pathways due to enzyme, compartment size, and/or ribosome availability limitations. ATP maintenance rate and in vivo apparent turnover numbers (k) were regressed from metabolic flux and protein concentration data to capture observed physiological growth yield and proteome efficiency and allocation, respectively. Estimated parameter values were found to vary with oxygen and nutrient availability. Overall, this work (i) provides condition-specific model parameters to recapitulate phenotypes corresponding to different extracellular environments, (ii) alludes to the enhancing effect of substrate channeling and post-translational activation on in vivo enzyme efficiency in glycolysis and electron transport chain, and (iii) reveals that the Crabtree effect is underpinned by specific limitations in mitochondrial proteome capacity and secondarily ribosome availability rather than overall proteome capacity.

摘要

酿酒酵母是一种重要的模式生物和生物生产的主力军。在这里,我们构建了一个紧凑且易于处理的基因组规模的资源平衡分析(RBA)模型(即命名为 scRBA),以便以计算有效的方式分析代谢通量和蛋白质组分配。资源能力模型(如 scRBA)提供了定量手段,可识别由于酶、隔室大小和/或核糖体可用性限制而导致生物合成途径中的瓶颈。通过代谢通量和蛋白质浓度数据回归 ATP 维持率和体内表观周转率(k),分别捕获观察到的生理生长产率和蛋白质组效率和分配。发现估计的参数值随氧气和营养物质的可用性而变化。总的来说,这项工作(i)提供了特定条件的模型参数,以重现对应于不同细胞外环境的表型,(ii)暗示了底物通道和翻译后激活对糖酵解和电子传递链中体内酶效率的增强作用,以及(iii)揭示了 Crabtree 效应是由线粒体蛋白质组能力的特定限制以及其次是核糖体可用性而不是整体蛋白质组能力所支撑的。

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