4.7 Article

No evidence for attenuated stress-induced extrastriatal dopamine signaling in psychotic disorder

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TRANSLATIONAL PSYCHIATRY
卷 5, 期 -, 页码 -

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NATURE PUBLISHING GROUP
DOI: 10.1038/tp.2015.37

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  1. ERC [309767-INTERACT]
  2. Maastricht University
  3. Network of European Neuroscience schools (NENS)
  4. South Limburg University fund (SWOL)
  5. Maastricht University post-doc Kootstra fellowship

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Stress is an important risk factor in the etiology of psychotic disorder. Preclinical work has shown that stress primarily increases dopamine (DA) transmission in the frontal cortex. Given that DA-mediated hypofrontality is hypothesized to be a cardinal feature of psychotic disorder, stress-related extrastriatal DA release may be altered in psychotic disorder. Here we quantified for the first time stress-induced extrastriatal DA release and the spatial extent of extrastriatal DA release in individuals with non-affective psychotic disorder (NAPD). Twelve healthy volunteers (HV) and 12 matched drug-free NAPD patients underwent a single infusion [F-18] fallypride positron emission tomography scan during which they completed the control and stress condition of the Montreal Imaging Stress Task. HV and NAPD did not differ in stress-induced [F-18] fallypride displacement and the spatial extent of stress-induced [F-18] fallypride displacement in medial prefrontal cortex (mPFC) and temporal cortex (TC). In the whole sample, the spatial extent of stress-induced radioligand displacement in right ventro-mPFC, but not dorso-mPFC or TC, was positively associated with task-induced subjective stress. Psychotic symptoms during the scan or negative, positive and general subscales of the Positive and Negative Syndrome Scale were not associated with stress-induced [F-18] fallypride displacement nor the spatial extent of stress-induced [F-18] fallypride displacement in NAPD. Our results do not offer evidence for altered stress-induced extrastriatal DA signaling in NAPD, nor altered functional relevance. The implications of these findings for the role of the DA system in NAPD and stress processing are discussed.

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