4.5 Article

Corticosterone administration targeting a hypo-reactive HPA axis rescues a socially-avoidant phenotype in scarcity-adversity reared rats

Journal

DEVELOPMENTAL COGNITIVE NEUROSCIENCE
Volume 40, Issue -, Pages -

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.dcn.2019.100716

Keywords

Social behavior; Social avoidance; CORT; Corticosterone; Cortisol; Development; Prefrontal cortex; Glucocorticoid; Hippocampus; Stress; Early-life adversity; Poverty; Scarcity; Hypocorticosteronism; Hypocortisolism; HPA axis

Funding

  1. National Science Foundation [1810208]
  2. National Science Foundation Graduate Research Graduate Research Fellowship Program [DGE-1137475]
  3. National Science Foundation Graduate Research Fellowship Program [DGE1342536]
  4. National Institute of Mental Health [R01-MH065635]
  5. Eunice Kennedy Shriver National Institute of Child Health and Human Development [R37-HD083217]
  6. SBE Off Of Multidisciplinary Activities
  7. Direct For Social, Behav & Economic Scie [1810208] Funding Source: National Science Foundation

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It is well-established that children from low-income, under-resourced families are at increased risk of altered social development. However, the biological mechanisms by which poverty-related adversities can get under the skin to influence social behavior are poorly understood and cannot be easily ascertained using human research alone. This study utilized a rodent model of scarcity-adversity, which encompasses material resource deprivation (scarcity) and reduced caregiving quality (adversity), to explore how early-life scarcity-adversity causally influences social behavior via disruption of developing stress physiology. Results showed that early-life scarcity-adversity exposure increased social avoidance when offspring were tested in a social approach test in periadolescence. Furthermore, early-life scarcity-adversity led to blunted hypothalamic-pituitary-adrenal (HPA) axis activity as measured via adrenocorticotropic hormone (ACTH) and corticosterone (CORT) reactivity following the social approach test. Western blot analysis of brain tissue revealed that glucocorticoid receptor levels in the dorsal (but not ventral) hippocampus and medial prefrontal cortex were significantly elevated in scarcity-adversity reared rats following the social approach test. Finally, pharmacological repletion of CORT in scarcity-adversity reared peri-adolescents rescued social behavior. Our findings provide causal support that early-life scarcity-adversity exposure negatively impacts social development via a hypocorticosteronism-dependent mechanism, which can be targeted via CORT administration to rescue social behavior.

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