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Article Dans Une Revue Molecular Biology and Evolution Année : 2009

Differential retention of metabolic genes following whole-genome duplication

Jean-François Gout
  • Fonction : Auteur
Laurent Duret

Résumé

Classical studies in Metabolic Control Theory have shown that metabolic fluxes usually exhibit little sensitivity to changes in individual enzyme activity, yet remain sensitive to global changes of all enzymes in a pathway. Therefore, little selective pressure is expected on the dosage or expression of individual metabolic genes, yet entire pathways should still be constrained. However, a direct estimate of this selective pressure had not been evaluated. Whole-genome duplications (WGDs) offer a good opportunity to address this question by analyzing the fates of metabolic genes during the massive gene losses that follow. Here, we take advantage of the successive rounds of WGD that occurred in the Paramecium lineage. We show that metabolic genes exhibit different gene retention patterns than nonmetabolic genes. Contrary to what was expected for individual genes, metabolic genes appeared more retained than other genes after the recent WGD, which was best explained by selection for gene expression operating on entire pathways. Metabolic genes also tend to be less retained when present at high copy number before WGD, contrary to other genes that show a positive correlation between gene retention and preduplication copy number. This is rationalized on the basis of the classical concave relationship relating metabolic fluxes with enzyme expression.

Domaines

Autre [q-bio.OT]

Dates et versions

hal-00428358 , version 1 (28-10-2009)
hal-00428358 , version 2 (08-10-2015)

Identifiants

Citer

Jean-François Gout, Laurent Duret, Daniel Kahn. Differential retention of metabolic genes following whole-genome duplication. Molecular Biology and Evolution, 2009, 26 (5), pp.1067-1072. ⟨10.1093/molbev/msp026⟩. ⟨hal-00428358v2⟩
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