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Imaging the neurobiological substrate of atypical depression by SPECT
Authors:Marco Pagani  Dario Salmaso  Davide Nardo  Cathrine Jonsson  Hans Jacobsson  Stig A. Larsson  Ann Gardner
Affiliation:(1) Institute of Cognitive Sciences and Technologies, CNR, Rome & Padua, Italy;(2) Department of Nuclear Medicine, Karolinska University Hospital, Stockholm, Sweden;(3) Department of Psychology, University of Rome La Sapienza, Rome, Italy;(4) Department of Radiology, Karolinska University Hospital, Stockholm, Sweden;(5) Karolinska Institutet, Department of Clinical Neuroscience, Section of Psychiatry, Karolinska University Hospital Huddinge, Stockholm, Sweden
Abstract:Purpose Neurobiological abnormalities underlying atypical depression have previously been suggested. The purpose of this study was to explore differences at functional brain imaging between depressed patients with and without atypical features and healthy controls. Methods Twenty-three out-patients with chronic depressive disorder recruited from a service for patients with audiological symptoms were investigated. Eleven fulfilled the DSM-IV criteria for atypical depression (mood reactivity and at least two of the following: weight gain, hypersomnia, leaden paralysis and interpersonal rejection sensitivity). Twenty-three healthy subjects served as controls. Voxel-based analysis was applied to explore differences in 99mTc-HMPAO uptake between groups. Results Patients in the atypical group had a higher prevalence of bilateral hearing impairment and higher depression and somatic distress ratings at the time of SPECT. Significantly higher tracer uptake was found bilaterally in the atypical group as compared with the non-atypicals in the sensorimotor (Brodmann areas, BA1–3) and premotor cortex in the superior frontal gyri (BA6), in the middle frontal cortex (BA8), in the parietal associative cortex (BA5, BA7) and in the inferior parietal lobule (BA40). Significantly lower tracer distribution was found in the right hemisphere in the non-atypicals compared with the controls in BA6, BA8, BA44, BA45 and BA46 in the frontal cortex, in the orbito-frontal cortex (BA11, BA47), in the postcentral parietal cortex (BA2) and in the multimodal association parietal cortex (BA40). Conclusion The differences found between atypical and non-atypical depressed patients suggest different neurobiological substrates in these patient groups. The putative links with the clinical features of atypical depression are discussed. These findings encourage the use of functional neuroimaging in psychiatric disorders.
Keywords:Atypical depression   99mTc-HMPAO  rCBF-SPECT  SPM  Unipolar depression
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