Role of norepinephrine in depression
by
Delgado PL, Moreno FA
Department of Psychiatry,
University of Arizona Medical Center,
Tucson, USA.
delgado@u.arizona.edu
J Clin Psychiatry 2000; 61 Suppl 1:5-12
ABSTRACT
This article reviews the role of norepinephrine (NE) and serotonin (5-HT) in
depression and the therapeutic effects of antidepressant drugs from the
perspective of human neurotransmitter depletion studies. The data reviewed
suggest that both noradrenergic and serotonergic systems are involved in
antidepressant action, but the specific impairment that underlies depression is
unclear and is likely to vary among patients. Results from neurotransmitter
depletion studies in depressed patients who have responded to treatment suggest
that, while interactions between NE and 5-HT are likely, neither of these 2
neurotransmitter systems is the final common pathway for the therapeutic effect
of antidepressant drugs. NE-selective antidepressant drugs appear to be
primarily dependent on the availability of NE for their effects. Likewise,
5-HT-selective antidepressants appear to be primarily dependent on the
availability of 5-HT for their effects. Antidepressants that cause effects on
both noradrenergic and serotonergic systems-such as mirtazapine-may be dependent
on the availability of both neurotransmitters for their effects. Neither 5-HT
nor NE depletion induced clinical depression in healthy subjects or worsened
depression in unmedicated symptomatic patients with major depression. This
finding suggests that the cause of depression is more complex than just an
alteration in the levels of 5-HT and/or NE. For some patients, depression may be
more directly caused by dysfunction in brain areas or neuronal systems modulated
by monoamine systems. We propose that antidepressant drugs may enhance
neurotransmission in normal noradrenergic or serotonergic neurons and, through a
time-dependent but as yet undiscovered process, restore function to brain areas
modulated by monoamine neurons. Future research should focus on understanding
the adaptive changes that follow enhancement of synaptic levels of monoamines in
neuronal circuits of the frontal cortex, amygdala, and hippocampus. Research
investigating the neurobiology of depression may be more informed if the focus
is shifted to investigating areas of the brain modulated by monoamine systems
rather than the monoamine systems themselves.
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