4.7 Article

Increased Stress-Induced Dopamine Release in Psychosis

Journal

BIOLOGICAL PSYCHIATRY
Volume 71, Issue 6, Pages 561-567

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.biopsych.2011.10.009

Keywords

Dopamine; neuroimaging; positron emission tomography; prodrome; schizophrenia; stress

Funding

  1. Canadian Institutes of Health Research (CIHR)
  2. Canada Foundation for Innovation
  3. Ontario Ministry of Research and Innovation
  4. Ontario Mental Health Foundation

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Background: A pathologic response to common life stressors, in which a hyperresponsive dopaminergic system is thought to play a key role, is a potential etiologic factor in the triggering and relapse of psychosis. However, there is no direct evidence that brain dopaminergic response to stress is exaggerated in psychosis. Methods: Using the ability of endogenous dopamine (DA) to compete with [C-11]-(+)-PHNO binding, as measured with positron emission tomography, we examined stress-induced DA release in response to a validated psychosocial stress task. We studied 12 clinical high-risk (CHR), 10 antipsychotic-naive subjects with schizophrenia (SCZ), and 12 matched healthy volunteers (HV). Stress-induced DA release was estimated as the percent change in binding potential between conditions (stress and control scan) in the striatal subdivisions: limbic striatum (LST), associative striatum (AST), and sensorimotor striatum (SMST). Results: We found a significant difference between groups in the AST (F = 8.13, df = 2,31, p = .001), and at the SMST (F = 3,64, df = 2,31, p = .03) but not in the LST (F = .43, df = 2,31, p = .40) with CHR and SCZ having larger [C-11]-(+)-PHNO displacement in response to the stress. Bonferroni-corrected comparisons confirmed that HV displacement (-2.86%) in the AST was significantly different in CHR (6.97%) and SCZ (11.44%) (with no significant difference between CHR and SCZ). Conclusions: This study reveals a sensitized dopaminergic response to stress in a psychiatric condition and may have important theoretical and clinical implications regarding efforts to abort or delay relapse and/or conversion to psychosis.

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