Abstract

Stress is accompanied by the activation of a number of endocrine secretions. Of these, adrenal glucocorticoids play a pivotal role as the principal regulators of the brain-pituitary response to stress and as agents which restore homeostatic balance and also protect the body from its own defense mechanisms such as inflammation and immune reactions. Though the body cannot long endure the absence of stress hormones, prolonged elevation of these hormones can have deleterious, even disastrous, effects such as increased susceptibility to infections and cancer. In addition the brain may also suffer in ways which are long-lasting and even permanent through glucocorticoid-induced neuronal loss and other long-term compensatory changes in neurochemical function which may influence mood and cognitive performance as well as the stress-response mechanism. This proposal investigates how prolonged stress and persistent and repeated elevation of glucocorticoid hormones alter neurochemistry of the principal adrenal steroid target area of the brain, the hippocampus, as well as of hormone sensitive areas of the limbic system and the frontal cortex. Having established glucocorticoid effects on glucocorticoid receptor levels, neurotransmitter receptor binding, cAMP formation stimulated by neurotransmitters, Synapsin I levels and mRNA and VIP levels and mRNA, we intend to investigate the degree to which effects of persistent and repeated glucocorticoid elevation (eg., 6-12 weeks duration) may be irreversible and reflect either the loss of cells or the compensatory response of the brain to cell loss. Finally, we shall determine whether the effects of repeated glucocorticoid elevation are cumulative or can be alleviated by periodic interruptions of stress hormone exposure. This work has relevance to degenerative brain diseases such as Alzheimer's endogenous depressive illness, and the study of persistent or chronic stress in loneliness, grieving, or isolation from normal life situations (eg., hostages, prisoners of war).

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
5R01MH041256-04
Application #
3379828
Study Section
(BPNB)
Project Start
1986-04-01
Project End
1991-03-31
Budget Start
1989-04-01
Budget End
1990-03-31
Support Year
4
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Rockefeller University
Department
Type
Graduate Schools
DUNS #
071037113
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Ryan, James D; Zhou, Yan; Contoreggi, Natalina H et al. (2018) Sex Differences in the Rat Hippocampal Opioid System After Oxycodone Conditioned Place Preference. Neuroscience 393:236-257
Gray, J D; Rubin, T G; Kogan, J F et al. (2018) Translational profiling of stress-induced neuroplasticity in the CA3 pyramidal neurons of BDNF Val66Met mice. Mol Psychiatry 23:904-913
Balsevich, Georgia; Sticht, Martin; Bowles, Nicole P et al. (2018) Role for fatty acid amide hydrolase (FAAH) in the leptin-mediated effects on feeding and energy balance. Proc Natl Acad Sci U S A 115:7605-7610
Marrocco, Jordan; Petty, Gordon H; RĂ­os, Mariel B et al. (2017) A sexually dimorphic pre-stressed translational signature in CA3 pyramidal neurons of BDNF Val66Met mice. Nat Commun 8:808
McEwen, Bruce S; Milner, Teresa A (2017) Understanding the broad influence of sex hormones and sex differences in the brain. J Neurosci Res 95:24-39
Lau, T; Bigio, B; Zelli, D et al. (2017) Stress-induced structural plasticity of medial amygdala stellate neurons and rapid prevention by a candidate antidepressant. Mol Psychiatry 22:227-234
McEwen, Bruce S (2017) Neurobiological and Systemic Effects of Chronic Stress. Chronic Stress (Thousand Oaks) 1:
McEwen, Bruce S (2016) In pursuit of resilience: stress, epigenetics, and brain plasticity. Ann N Y Acad Sci 1373:56-64
McEwen, Bruce S (2016) Stress-induced remodeling of hippocampal CA3 pyramidal neurons. Brain Res 1645:50-4
Hunter, Richard G; Seligsohn, Ma'ayan; Rubin, Todd G et al. (2016) Stress and corticosteroids regulate rat hippocampal mitochondrial DNA gene expression via the glucocorticoid receptor. Proc Natl Acad Sci U S A 113:9099-104

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