Frontiers in Endocrinology (Nov 2014)

Immediate effects of maternal deprivation on the (re)activity of the HPA axis differ in CD1 and C57Bl/6J mouse pups

  • Nikolaos P Daskalakis,
  • Nikolaos P Daskalakis,
  • Nikolaos P Daskalakis,
  • Leo eEnthoven,
  • Edwige eSchoonheere,
  • Edo Ronald De Kloet,
  • Edo Ronald De Kloet,
  • Melly S Oitzl,
  • Melly S Oitzl

DOI
https://doi.org/10.3389/fendo.2014.00190
Journal volume & issue
Vol. 5

Abstract

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The postnatal development of the mouse is characterised by a period of hypo-responsiveness of the hypothalamic-pituitary-adrenal (HPA) axis to mild stressors. Maternal deprivation (MD) during this period can disrupt the quiescence of the HPA-axis. The present study examined the influence of strain (outbred CD1 versus inbred C57BL/6J mice) on some central and peripheral components of the HPA-axis in neonatal mice (5 day-old) in the presence of their mother or after 24 h MD (on postnatal day 4) under basal or mild stressful conditions. In the presence of the dam, adrenal corticosterone (CORT) secretion was low in both mouse strains. Compared to CD1 mice, C57BL/6J had lower CORT levels associated with higher ACTH levels and ACTH/CORT ratio (i.e., lower adrenal sensitivity to ACTH), and higher glucocorticoid receptor (GR) mRNA expression in the paraventricular nucleus. Although MD disinhibited the HPA-axis in both strains as reflected by increased basal CORT and ACTH, we found a strain-dependent pattern. MD increased CORT more in C57BL/6J, compared to CD1 mice, together with a lower ACTH/CORT ratio (i.e., higher adrenal sensitivity to ACTH), while GR mRNA was no longer different in the two strains. However, this increased adrenal sensitivity in maternally deprived C57BL/6J mice was not reflected in their CORT response to a subsequent novelty stressor, possibly due to a MD-induced ceiling effect in their steroidogenic capacity.In conclusion, the immediate outcome of MD depends on the genetic background of the mother-infant dyad, suggesting that maybe also the outcome in later-life cannot be generalized. genetic background of the mother-infant dyad, predicting that the outcome in later-life cannot be generalized.

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