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同位素非稳态代谢通量分析(INST-MFA):将理论付诸实践。

Isotopically nonstationary metabolic flux analysis (INST-MFA): putting theory into practice.

机构信息

Department of Chemical and Biomolecular Engineering, Vanderbilt University, PMB 351604, Nashville, TN 37235-1604, USA.

Department of Chemical and Biomolecular Engineering, Vanderbilt University, PMB 351604, Nashville, TN 37235-1604, USA; Department of Molecular Physiology and Biophysics, Vanderbilt University, PMB 351604, Nashville, TN 37235-1604, USA.

出版信息

Curr Opin Biotechnol. 2018 Dec;54:80-87. doi: 10.1016/j.copbio.2018.02.013. Epub 2018 Mar 6.

Abstract

Typically, C flux analysis relies on assumptions of both metabolic and isotopic steady state. If metabolism is steady but isotope labeling is not allowed to fully equilibrate, isotopically nonstationary metabolic flux analysis (INST-MFA) can be used to estimate fluxes. This requires solution of differential equations that describe the time-dependent labeling of network metabolites, while iteratively adjusting the flux and pool size parameters to match the transient labeling measurements. INST-MFA holds a number of unique advantages over approaches that rely solely upon steady-state isotope enrichments. First, INST-MFA can be applied to estimate fluxes in autotrophic systems, which consume only single-carbon substrates. Second, INST-MFA is ideally suited to systems that label slowly due to the presence of large intermediate pools or pathway bottlenecks. Finally, INST-MFA provides increased measurement sensitivity to estimate reversible exchange fluxes and metabolite pool sizes, which represents a potential framework for integrating metabolomic analysis with C flux analysis. This review highlights the unique capabilities of INST-MFA, describes newly available software tools that automate INST-MFA calculations, presents several practical examples of recent INST-MFA applications, and discusses the technical challenges that lie ahead.

摘要

通常情况下,C 通量分析依赖于代谢和同位素稳态的假设。如果代谢是稳定的,但不允许同位素标记完全达到平衡,那么可以使用同位素非稳态代谢通量分析(INST-MFA)来估计通量。这需要求解描述网络代谢物随时间变化的标记的微分方程,同时迭代调整通量和池大小参数以匹配瞬态标记测量值。与仅依赖于稳态同位素富集的方法相比,INST-MFA 具有许多独特的优势。首先,INST-MFA 可用于估算仅消耗单碳底物的自养系统中的通量。其次,由于存在大的中间池或途径瓶颈,INST-MFA 非常适合标记缓慢的系统。最后,INST-MFA 提高了对可逆交换通量和代谢物池大小的测量灵敏度,这代表了将代谢组学分析与 C 通量分析相结合的潜在框架。本文综述了 INST-MFA 的独特功能,描述了新的可用软件工具,这些工具可自动进行 INST-MFA 计算,展示了最近 INST-MFA 应用的几个实际示例,并讨论了未来的技术挑战。

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