PLoS ONE (Jan 2015)

Developmental Expression and Glucocorticoid Control of the Leptin Receptor in Fetal Ovine Lung.

  • Miles J De Blasio,
  • Maria Boije,
  • Owen R Vaughan,
  • Brett S Bernstein,
  • Katie L Davies,
  • Alice Plein,
  • Sarah L Kempster,
  • Gordon C S Smith,
  • D Stephen Charnock-Jones,
  • Dominique Blache,
  • F B Peter Wooding,
  • Dino A Giussani,
  • Abigail L Fowden,
  • Alison J Forhead

DOI
https://doi.org/10.1371/journal.pone.0136115
Journal volume & issue
Vol. 10, no. 8
p. e0136115

Abstract

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The effects of endogenous and synthetic glucocorticoids on fetal lung maturation are well-established, although the role of leptin in lung development before birth is unclear. This study examined mRNA and protein levels of the signalling long-form leptin receptor (Ob-Rb) in fetal ovine lungs towards term, and after experimental manipulation of glucocorticoid levels in utero by fetal cortisol infusion or maternal dexamethasone treatment. In fetal ovine lungs, Ob-Rb protein was localised to bronchiolar epithelium, bronchial cartilage, vascular endothelium, alveolar macrophages and type II pneumocytes. Pulmonary Ob-Rb mRNA abundance increased between 100 (0.69 fractional gestational age) and 144 days (0.99) of gestation, and by 2-4-fold in response to fetal cortisol infusion and maternal dexamethasone treatment. In contrast, pulmonary Ob-Rb protein levels decreased near term and were halved by glucocorticoid treatment, without any significant change in phosphorylated signal transducer and activator of transcription-3 (pSTAT3) at Ser727, total STAT3 or the pulmonary pSTAT3:STAT3 ratio. Leptin mRNA was undetectable in fetal ovine lungs at the gestational ages studied. These findings demonstrate differential control of pulmonary Ob-Rb transcript abundance and protein translation, and/or post-translational processing, by glucocorticoids in utero. Localisation of Ob-Rb in the fetal ovine lungs, including alveolar type II pneumocytes, suggests a role for leptin signalling in the control of lung growth and maturation before birth.