Open Biology (Sep 2022)

Prenatal transcript levels and metabolomics analyses reveal metabolic changes associated with intrauterine growth restriction and sex

  • Siriluck Ponsuksili,
  • Eduard Murani,
  • Frieder Hadlich,
  • Muhammad Arsalan Iqbal,
  • Beate Fuchs,
  • Christina E. Galuska,
  • Alvaro Perdomo-Sabogal,
  • Fabio Sarais,
  • Nares Trakooljul,
  • Henry Reyer,
  • Michael Oster,
  • Klaus Wimmers

DOI
https://doi.org/10.1098/rsob.220151
Journal volume & issue
Vol. 12, no. 9

Abstract

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The metabolic changes associated with intrauterine growth restriction (IUGR) particularly affect the liver, which is a central metabolic organ and contributes significantly to the provision of energy and specific nutrients and metabolites. Therefore, our aim was to decipher and elucidate the molecular pathways of developmental processes mediated by miRNAs and mRNAs, as well as the metabolome in fetal liver tissue in IUGR compared to appropriate for gestational age groups (AGA). Discordant siblings representing the extremes in fetal weight at day 63 post conception (dpc) were selected from F2 fetuses of a cross of German Landrace and Pietrain. Most of the changes in the liver of IUGR at midgestation involved various lipid metabolic pathways, both on transcript and metabolite levels, especially in the category of sphingolipids and phospholipids. Differentially expressed miRNAs, such as miR-34a, and their differentially expressed mRNA targets were identified. Sex-specific phenomena were observed at both the transcript and metabolite levels, particularly in male. This suggests that sex-specific adaptations in the metabolic system occur in the liver during midgestation (63 dpc). Our multi-omics network analysis reveals interactions and changes in the metabolic system associated with IUGR and identified an important biosignature that differs between IUGR and AGA piglets.

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