Cycling of co-substrates, whereby a metabolite is converted among alternate forms via different reactions, is ubiquitous in metabolism. Several cycled co-substrates are well known as energy and electron carriers (e.g. ATP and NAD(P)H), but there are also other metabolites that act as cycled co-substrates in different parts of central metabolism. Here, we develop a mathematical framework to analyse the effect of co-substrate cycling on metabolic flux. In the cases of a single reaction and linear pathways, we find that co-substrate cycling imposes an additional flux limit on a reaction, distinct to the limit imposed by the kinetics of the primary enzyme catalysing that reaction. Using analytical methods, we show that this additional limit is a function of the total pool size and turnover rate of the cycled co-substrate. Expanding from this insight and using simulations, we show that regulation of these two parameters can allow regulation of flux dynamics in branched and coupled pathways. To support these theoretical insights, we analysed existing flux measurements and enzyme levels from the central carbon metabolism and identified several reactions that could be limited by the dynamics of co-substrate cycling. We discuss how the limitations imposed by co-substrate cycling provide experimentally testable hypotheses on specific metabolic phenotypes. We conclude that measuring and controlling co-substrate dynamics is crucial for understanding and engineering metabolic fluxes in cells.
Keywords: A. thaliana; E. coli; S. cerevisiae; computational biology; human; systems biology.
Metabolism powers individual cells and ultimately the body. It comprises a sequence of chemical reactions that cells use to break down substances and generate energy. These reactions are catalyzed by enzymes, which are proteins that speed up the rate of the reaction. Many reactions also involve co-substrates, which are themselves transformed by individual reactions but are eventually converted back into their original form in a series of steps. This process is known as co-substrate cycling. Scientists have long been interested in understanding what controls the rate at which metabolic reactions and metabolic pathways convert a substance into a final product. This is a difficult subject to study because of the complexity of the metabolic pathways, with their branched, linear or coupled structures. In the past, researchers have looked at the influence of enzymes on the rate of a metabolic pathway, but less has been known about the effect of co-substrate cycling. To find out more, West, Delattre et al. developed a series of mathematical models to describe different types of metabolic pathways in terms of the number of metabolites that enter and leave it, including the influence of co-substrates. They found that co-substrate cycling, when involved in a metabolic reaction, limits the speed with which the reaction happens. This is distinct from the limit that enzymes impose on the speed of the reaction. It depends on the total amount of co-substrates in the cell: changing the number of co-substrates in the cell influences the speed at which the metabolic reaction takes place. This study has increased our understanding of how metabolic pathways work, and what controls the speed at which reactions take place. It opens up a new potential method for explaining how cells control metabolic reaction rates and how metabolic substrates can be directed across different pathways. This research is likely to inspire future research into the influence of co-substrates in different cell types and conditions.
© 2023, West, Delattre et al.