International Journal of Molecular Sciences (Jan 2024)

Placenta-Specific Transcripts Containing Androgen Response Elements Are Altered In Silico by Male Growth Outcomes

  • Ashley S. Meakin,
  • Melanie Smith,
  • Janna L. Morrison,
  • Claire T. Roberts,
  • Martha Lappas,
  • Stacey J. Ellery,
  • Olivia Holland,
  • Anthony Perkins,
  • Sharon A. McCracken,
  • Vicki Flenady,
  • Vicki L. Clifton

DOI
https://doi.org/10.3390/ijms25031688
Journal volume & issue
Vol. 25, no. 3
p. 1688

Abstract

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A birthweight centile (BWC) below the 25th is associated with an elevated risk of adverse perinatal outcomes, particularly among males. This male vulnerability may stem from alterations in placenta-specific androgen signalling, a signalling axis that involves the androgen receptor (AR)-mediated regulation of target genes containing androgen response elements (AREs). In this study, we examined global and ARE-specific transcriptomic signatures in term male placentae (≥37 weeks of gestation) across BWC subcategories (30th) using RNA-seq and gene set enrichment analysis. ARE-containing transcripts in placentae with BWCs below the 10th percentile were upregulated compared to those in the 10th–30th and >30th percentiles, which coincided with the enrichment of gene sets related to hypoxia and the suppression of gene sets associated with mitochondrial function. In the absence of ARE-containing transcripts in silico, 30th BWC subcategory. Collectively, our in silico findings suggest that changes in the expression of ARE-containing transcripts in male placentae may contribute to impaired placental vasculature and therefore result in reduced fetal growth outcomes.

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