stochasticity in protein levels drives colinearity of gene order in metabolic operons of escherichia coli特性转化在蛋白质水平驱动器同线性大肠杆菌的代谢操纵子基因秩序.pdfVIP
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stochasticity in protein levels drives colinearity of gene order in metabolic operons of escherichia coli特性转化在蛋白质水平驱动器同线性大肠杆菌的代谢操纵子基因秩序
Stochasticity in Protein Levels Drives Colinearity of Gene
Order in Metabolic Operons of Escherichia coli
´ ´ 1 2 ´ 1
Karoly Kovacs , Laurence D. Hurst *, Balazs Papp *
1 Institute of Biochemistry, Biological Research Center, Szeged, Hungary, 2 Department of Biology and Biochemistry, University of Bath, Bath, United Kingdom
Abstract
In bacterial genomes, gene order is not random. This is most evident when looking at operons, these often encoding
enzymes involved in the same metabolic pathway or proteins from the same complex. Is gene order within operons
nonrandom, however, and if so why? We examine this issue using metabolic operons as a case study. Using the metabolic
network of Escherichia coli, we define the temporal order of reactions. We find a pronounced trend for genes to appear in
operons in the same order as they are needed in metabolism (colinearity). This is paradoxical as, at steady state, enzymes
abundance should be independent of order within the operon. We consider three extensions of the steady-state model that
could potentially account for colinearity: (1) increased productivity associated with higher expression levels of the most 59
genes, (2) a faster metabolic processing immediately after up-regulation, and (3) metabolic stalling owing to stochastic
protein loss. We establish the validity of these hypotheses by employing deterministic and stochastic models of enzyme
kinetics. The stochastic stalling hypothesis correctly and uniquely predicts that colinearity is more pronounced both for
lowly expressed operons and for genes that are not physically adjacent. The alternative models fail to find any support.
These results support the view that stochasticity is a pervasive problem to a cell and that gene order evol
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