Nature Communications (Jun 2024)

Pulmonary maternal immune activation does not cross the placenta but leads to fetal metabolic adaptation

  • Signe Schmidt Kjølner Hansen,
  • Robert Krautz,
  • Daria Rago,
  • Jesper Havelund,
  • Arnaud Stigliani,
  • Nils J. Færgeman,
  • Audrey Prézelin,
  • Julie Rivière,
  • Anne Couturier-Tarrade,
  • Vyacheslav Akimov,
  • Blagoy Blagoev,
  • Betina Elfving,
  • Ditte Neess,
  • Ulla Vogel,
  • Konstantin Khodosevich,
  • Karin Sørig Hougaard,
  • Albin Sandelin

DOI
https://doi.org/10.1038/s41467-024-48492-x
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 24

Abstract

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Abstract The fetal development of organs and functions is vulnerable to perturbation by maternal inflammation which may increase susceptibility to disorders after birth. Because it is not well understood how the placenta and fetus respond to acute lung- inflammation, we characterize the response to maternal pulmonary lipopolysaccharide exposure across 24 h in maternal and fetal organs using multi-omics, imaging and integrative analyses. Unlike maternal organs, which mount strong inflammatory immune responses, the placenta upregulates immuno-modulatory genes, in particular the IL-6 signaling suppressor Socs3. Similarly, we observe no immune response in the fetal liver, which instead displays metabolic changes, including increases in lipids containing docosahexaenoic acid, crucial for fetal brain development. The maternal liver and plasma display similar metabolic alterations, potentially increasing bioavailability of docosahexaenoic acid for the mother and fetus. Thus, our integrated temporal analysis shows that systemic inflammation in the mother leads to a metabolic perturbation in the fetus.