Whole-cell modeling in yeast predicts compartment-specific proteome constraints that drive metabolic strategies

Author:

Elsemman Ibrahim E.ORCID,Prado Angelica Rodriguez,Grigaitis PranasORCID,Albornoz Manuel GarciaORCID,Harman VictoriaORCID,Holman Stephen W.ORCID,van Heerden JohanORCID,Bruggeman Frank J.ORCID,Bisschops Mark M.M.,Sonnenschein NikolausORCID,Hubbard SimonORCID,Beynon Rob,Daran-Lapujade PascaleORCID,Nielsen JensORCID,Teusink BasORCID

Abstract

When conditions change, unicellular organisms rewire their metabolism to sustain cell maintenance and cellular growth. Such rewiring may be understood as resource re-allocation under cellular constraints. Eukaryal cells contain metabolically active organelles such as mitochondria, competing for cytosolic space and resources, and the nature of the relevant cellular constraints remain to be determined for such cells. Here we developed a comprehensive metabolic model of the yeast cell, based on its full metabolic reaction network extended with protein synthesis and degradation reactions (16304 reactions in total). The model predicts metabolic fluxes and corresponding protein expression by constraining compartment-specific protein pools and maximising growth rate. Comparing model predictions with quantitative experimental data revealed that under glucose limitation, a mitochondrial constraint limits growth at the onset of ethanol formation - known as the Crabtree effect. Under sugar excess, however, a constraint on total cytosolic volume dictates overflow metabolism. Our comprehensive model thus identifies condition-dependent and compartment-specific constraints that can explain metabolic strategies and protein expression profiles from growth rate optimization, providing a framework to understand metabolic adaptation in eukaryal cells.

Publisher

Cold Spring Harbor Laboratory

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