PLoS Computational Biology (Nov 2011)

Transcriptomic coordination in the human metabolic network reveals links between n-3 fat intake, adipose tissue gene expression and metabolic health.

  • Melissa J Morine,
  • Audrey C Tierney,
  • Ben van Ommen,
  • Hannelore Daniel,
  • Sinead Toomey,
  • Ingrid M F Gjelstad,
  • Isobel C Gormley,
  • Pablo Pérez-Martinez,
  • Christian A Drevon,
  • Jose López-Miranda,
  • Helen M Roche

DOI
https://doi.org/10.1371/journal.pcbi.1002223
Journal volume & issue
Vol. 7, no. 11
p. e1002223

Abstract

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Understanding the molecular link between diet and health is a key goal in nutritional systems biology. As an alternative to pathway analysis, we have developed a joint multivariate and network-based approach to analysis of a dataset of habitual dietary records, adipose tissue transcriptomics and comprehensive plasma marker profiles from human volunteers with the Metabolic Syndrome. With this approach we identified prominent co-expressed sub-networks in the global metabolic network, which showed correlated expression with habitual n-3 PUFA intake and urinary levels of the oxidative stress marker 8-iso-PGF(2α). These sub-networks illustrated inherent cross-talk between distinct metabolic pathways, such as between triglyceride metabolism and production of lipid signalling molecules. In a parallel promoter analysis, we identified several adipogenic transcription factors as potential transcriptional regulators associated with habitual n-3 PUFA intake. Our results illustrate advantages of network-based analysis, and generate novel hypotheses on the transcriptomic link between habitual n-3 PUFA intake, adipose tissue function and oxidative stress.