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Detecting and investigating substrate cycles in a genome‐scale human metabolic network
Author(s) -
Gebauer Juliane,
Schuster Stefan,
de Figueiredo Luís F.,
Kaleta Christoph
Publication year - 2012
Publication title -
the febs journal
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.981
H-Index - 204
eISSN - 1742-4658
pISSN - 1742-464X
DOI - 10.1111/j.1742-4658.2012.08700.x
Subject(s) - substrate (aquarium) , flux (metallurgy) , metabolism , fructose , energy metabolism , enzyme , cofactor , biochemistry , chemistry , biology , biophysics , ecology , organic chemistry , endocrinology
Substrate cycles, also known as futile cycles, are cyclic metabolic routes that dissipate energy by hydrolysing cofactors such as ATP. They were first described to occur in the muscles of bumblebees and brown adipose tissue in the 1970s. A popular example is the conversion of fructose 6‐phosphate to fructose 1,6‐bisphosphate and back. In the present study, we analyze a large number of substrate cycles in human metabolism that consume ATP and discuss their statistics. For this purpose, we use two recently published methods (i.e. EFMEvolver and the K ‐shortest EFM method) to calculate samples of 100 000 and 15 000 substrate cycles, respectively. We find an unexpectedly high number of substrate cycles in human metabolism, with up to 100 reactions per cycle, utilizing reactions from up to six different compartments. An analysis of tissue‐specific models of liver and brain metabolism shows that there is selective pressure that acts against the uncontrolled dissipation of energy by avoiding the coexpression of enzymes belonging to the same substrate cycle. This selective force is particularly strong against futile cycles that have a high flux as a result of thermodynamic principles.

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