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The Journal of Neuroscience, September 15, 2000, 20(18):6983-6988
Neurobiological Correlates of Individual Differences in
Novelty-Seeking Behavior in the Rat: Differential Expression of
Stress-Related Molecules
M.
Kabbaj1,
D. P.
Devine3,
V. R.
Savage2, and
H.
Akil1
1 Mental Health Research Institute and
2 Department of Psychology, University of Michigan, Ann
Arbor, Michigan 48109-0720, and 3 Department of Psychology,
University of Florida, Gainesville, Florida 32611-2250
It is well established that individual rats exhibit marked
differences in behavioral responses to a novel environment. Rats that
exhibit high rates of locomotor activity and sustained exploration in
such an environment also exhibit high concentrations of stress-induced plasma corticosterone, linking this behavior to the stress system. Furthermore, these high-responding (HR) rats, in contrast to their low-responding (LR) counterparts, have a greater propensity to self-administer drugs. Thus, HR rats have been described as
"novelty" seeking in that they are more active and explore novel
stimuli more vigorously, despite the fact that this elicits in them
high stress responses. In this study, we have further characterized the
behavior of HR and LR rats in tests of anxiety and characterized their
stress responses to either experimenter- or self-imposed stressors. We
then investigated the physiological basis of these individual
differences, focusing on stress-related molecules, including the
glucocorticoid receptor (GR), the mineralocorticoid receptor (MR),
corticotropin-releasing hormone (CRH) and pro-opiomelanocortin (POMC)
in the context of the limbic-hypothalamo-pituitary adrenal axis. We
have found that HR rats did not differ from LR in their basal
expression of POMC in the pituitary. However, HR rats exhibited higher
levels of CRH mRNA in the hypothalamic paraventricular nucleus but
lower basal levels in the central nucleus of the amygdala. The basal
expression of hippocampal MR is not different between HR and LR rats.
Interestingly, the basal expression of hippocampal GR mRNA is
significantly lower in HR than in LR rats. This low level of
hippocampal GR expression in HR rats appears to be responsible, at
least in part, for their decreased anxiety in exploring novelty. Indeed, the anxiety level of LR rats becomes similar to HR rats after
the administration into the hippocampus of a GR antagonist, RU38486.
These data indicate that basal differences in gene expression of key
stress-related molecules may play an important role in determining
individual differences in responsiveness to stress and novelty. They
point to a new role of hippocampal GR, strongly implicating this
receptor in determining individual differences in anxiety and
novelty-seeking behavior.
Key words:
anxiety; drug addiction; reactivity to novelty; novelty
seeking; stress; individual differences
Copyright © 2000 Society for Neuroscience 0270-6474/00/20186983-06$05.00/0
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