Decrease in brain serotonin 2 receptor binding in patients with major
depression following desipramine treatment: a positron emission tomography study
with fluorine-18-labeled setoperone
by
Yatham LN, Liddle PF, Dennie J, Shiah IS,
Adam MJ, Lane CJ, Lam RW, Ruth
TJ
Division of Mood Disorders,
The University of British Columbia,
Vancouver,
Canada.
yatham@unixg.ubc.ca
Arch Gen Psychiatry 1999 Aug; 56(8):705-11
ABSTRACT
BACKGROUND: The neuroreceptor changes involved in therapeutic efficacy of
various antidepressants remain unclear. Preclinical studies have shown that
long-term administration of various antidepressants causes down-regulation of
brain serotonin 2 (5-HT2) receptors in rodents, but it is unknown if similar
changes occur following antidepressant treatment in depressed patients. Our
purpose, therefore, was to assess the effects of treatment with desipramine
hydrochloride on brain 5-HT2 receptors in depressed patients using positron
emission tomography (PET) and fluorine-18 (18F)-labeled setoperone. METHODS:
Eleven patients who met DSM-IV criteria for major depression as determined by a
structured clinical interview for DSM-III-R diagnosis and suitable for treatment
with desipramine were recruited. Ten patients underwent a PET scan before and
another after 3 to 4 weeks of treatment with desipramine. RESULTS: Eight of the
10 patients responded to desipramine treatment as indicated by more than 50%
decrease in Hamilton Depression Rating Scale scores. Depressed patients showed a
significant decrease in 5-HT2 receptor binding as measured by setoperone binding
in frontal, temporal, parietal, and occipital cortical regions following
desipramine treatment. The decrease in 5-HT2 receptor binding was observed
bilaterally and was particularly prominent in frontal cortex. CONCLUSIONS:
Depressed patients showed a significant reduction in available 5-HT2 receptors
in the brain following desipramine treatment, but it is unknown if this change
in 5-HT2 receptors is due to clinical improvement or an effect of desipramine
that is unrelated to clinical status.
5-HT2
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