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On Site Link: CRF and Unipolar Depression Gold
PW, Chrousos GP.
Organization of the stress system and its dysregulation
in melancholic and atypical depression: high vs low CRH/NE states.
Mol Psychiatry 2002;7(3):254-75
"Stress precipitates depression and alters
its natural history. Major depression and the stress response share similar phenomena,
mediators and circuitries. Thus, many of the features of major depression potentially
reflect dysregulations of the stress response. The stress response itself consists
of alterations in levels of anxiety, a loss of cognitive and affective flexibility,
activation of the hypothalamic-pituitary-adrenal (HPA) axis and autonomic nervous
system, and inhibition of vegetative processes that are likely to impede survival
during a life-threatening situation (eg sleep, sexual activity, and endocrine
programs for growth and reproduction). Because depression is a heterogeneous illness,
we studied two diagnostic subtypes, melancholic and atypical depression. In melancholia,
the stress response seems hyperactive, and patients are anxious, dread the future,
lose responsiveness to the environment, have insomnia, lose their appetite, and
a diurnal variation with depression at its worst in the morning. They also have
an activated CRH system and may have diminished activities of the growth hormone
and reproductive axes. Patients with atypical depression present with a syndrome
that seems the antithesis of melancholia. They are lethargic, fatigued, hyperphagic,
hypersomnic, reactive to the environment, and show diurnal variation of depression
that is at its best in the morning. In contrast to melancholia, we have advanced
several lines of evidence of a down-regulated hypothalamic-pituitary adrenal axis
and CRH deficiency in atypical depression, and our data show us that these are
of central origin. Given the diversity of effects exerted by CRH and cortisol,
the differences in melancholic and atypical depression suggest that studies of
depression should examine each subtype separately. In the present paper, we shall
first review the mediators and circuitries of the stress system to lay the groundwork
for placing in context physiologic and structural alterations in depression that
may occur as part of stress system dysfunction." [PDF]
[Note that the authors use the atypical acronym CRH rather than the equivalent
acronym CRF.] Bissette G, Klimek V, Pan J, Stockmeier
C, Ordway G.
Elevated concentrations of CRF in the locus coeruleus
of depressed subjects.
Neuropsychopharmacology. 2003 Jul;28(7):1328-35.
Epub 2003 May 21.
"Research evidence that corticotropin-releasing factor
(CRF) plays a role in the pathophysiology of major depressive disorder (MDD) has
accumulated over the past 20 years. The elevation of lumbar cerebrospinal fluid
(CSF) concentrations of CRF decreased responsiveness of pituitary CRF receptors
to challenge with synthetic CRF, and increased levels of serum cortisol in MDD
subjects support the hypothesis that CRF is chronically hypersecreted in at least
the endocrine circuits of the hypothalamic-pituitary-adrenal (HPA) axis and may
also involve other CRF brain circuits mediating emotional responses and/or arousal.
One such circuit includes the excitatory CRF input to the locus coeruleus (LC),
the major source of norepinephrine in the brain. Furthermore, there are now reports
of decreased levels of CRF in lumbar CSF from MDD patients after symptom relief
from chronic treatment with antidepressant drugs or electroconvulsive therapy.
Whether this normalization reflects therapeutic effects on both endocrine- and
limbic-associated CRF circuits has not yet been effectively addressed. In this
brief report, we describe increased concentrations of CRF-like immunoreactivity
in micropunches of post-mortem LC from subjects with MDD symptoms as established
by retrospective psychiatric diagnosis compared to nondepressed subjects matched
for age and sex." [Abstract] Austin
MC, Janosky JE, Murphy HA.
Increased corticotropin-releasing hormone
immunoreactivity in monoamine-containing pontine nuclei of depressed suicide men.
Mol
Psychiatry. 2003 Mar;8(3):324-32.
"A number of clinical investigations
and postmortem brain studies have provided evidence that excessive corticotropin-releasing
hormone (CRH) secretion and neurotransmission is involved in the pathophysiology
of depressive illness, and several studies have suggested that the hyperactivity
in CRH neurotransmission extends beyond the hypothalamus involving several extra-hypothalamic
brain regions. The present study was designed to test the hypothesis that CRH
levels are increased in specific brainstem regions of suicide victims with a diagnosis
of major depression. Frozen tissue sections of the pons containing the locus coeruleus
and caudal raphe nuclei from 11 matched pairs of depressed suicide and control
male subjects were processed for radioimmunocytochemistry using a primary antiserum
to CRH and a ([125])I-IgG secondary antibody. The optical density corresponding
to the level of CRH-immunoreactivity (IR) was quantified in specific pontine regions
from the film autoradiographic images. The level of CRH-IR was increased by 30%
in the locus coeruleus, 39% in the median raphe and 45% in the caudal dorsal raphe
in the depressed suicide subjects compared to controls. No difference in CRH-IR
was found in the dorsal tegmentum or medial parabrachial nucleus between the subject
groups. These findings reveal that CRH-IR levels are specifically increased in
norepinephrine- and serotonin-containing pontine nuclei of depressed suicide men,
and thus they are consistent with the hypothesis that CRH neurotransmission is
elevated in extra-hypothalamic brain regions of depressed subjects." [Abstract] Bissette
G, Klimek V, Pan J, Stockmeier C, Ordway G.
Elevated Concentrations
of CRF in the Locus Coeruleus of Depressed Subjects.
Neuropsychopharmacology.
2003 Jul;28(7):1328-35.
"Research evidence that corticotropin-releasing
factor (CRF) plays a role in the pathophysiology of major depressive disorder
(MDD) has accumulated over the past 20 years. The elevation of lumbar cerebrospinal
fluid (CSF) concentrations of CRF decreased responsiveness of pituitary CRF receptors
to challenge with synthetic CRF, and increased levels of serum cortisol in MDD
subjects support the hypothesis that CRF is chronically hypersecreted in at least
the endocrine circuits of the hypothalamic-pituitary-adrenal (HPA) axis and may
also involve other CRF brain circuits mediating emotional responses and/or arousal.
One such circuit includes the excitatory CRF input to the locus coeruleus (LC),
the major source of norepinephrine in the brain. Furthermore, there are now reports
of decreased levels of CRF in lumbar CSF from MDD patients after symptom relief
from chronic treatment with antidepressant drugs or electroconvulsive therapy.
Whether this normalization reflects therapeutic effects on both endocrine- and
limbic-associated CRF circuits has not yet been effectively addressed. In this
brief report, we describe increased concentrations of CRF-like immunoreactivity
in micropunches of post-mortem LC from subjects with MDD symptoms as established
by retrospective psychiatric diagnosis compared to nondepressed subjects matched
for age and sex." [Abstract] Zhu
MY, Klimek V, Dilley GE, Haycock JW, Stockmeier C, Overholser JC, Meltzer HY,
Ordway GA.
Elevated levels of tyrosine hydroxylase in the locus coeruleus
in major depression.
Biol Psychiatry. 1999 Nov 1;46(9):1275-86.
"BACKGROUND:
Levels of tyrosine hydroxylase (TH) are regulated in the noradrenergic locus coeruleus
(LC) in response to changes in the activity of LC neurons and in response to changes
in brain levels of norepinephrine. To study the potential role of central noradrenergic
neurons in the pathobiology of major depression, TH protein was measured in the
LC from postmortem brains of 13 subjects with a diagnosis of major depression
and 13 age-matched control subjects having no Axis I psychiatric diagnosis. Most
of the major depressive subjects died as a result of suicide. METHODS: Protein
from sections cut through multiple rostro-caudal levels of LC was transferred
to Immobilon-P membrane, immunoblotted for TH, and quantified autoradiographically.
RESULTS: The distribution of TH-immunoreactivity (TH-ir) along the rostro-caudal
axis of the LC was uneven and was paralleled by a similar uneven distribution
of neuromelanin-containing cells in both major depressive and psychiatrically
normal control subjects. Amounts of TH-ir in the rostral, middle and caudal levels
of the LC from major depressive subjects were significantly higher than that of
matched control subjects. There were no significant differences in the number
of noradrenergic cells at any particular level of the LC comparing major depressive
subjects to control subjects. CONCLUSIONS: Elevated expression of TH in the LC
in major depression implies a premortem overactivity of these neurons, or a deficiency
of the cognate transmitter, norepinephrine." [Abstract] Ordway
GA, Smith KS, Haycock JW.
Elevated tyrosine hydroxylase in the locus
coeruleus of suicide victims.
J Neurochem. 1994 Feb;62(2):680-5.
"The
amounts of tyrosine hydroxylase protein in locus coeruleus from nine pairs of
antidepressant-free suicide victims and age-matched, sudden-death control cases
were determined by quantitative blot immunolabeling of cryostat-cut sections from
the caudal portion of the nucleus. In each of the nine age-matched pairs, the
concentration of tyrosine hydroxylase was greater in the sample from the suicide
victim, with values ranging from 108 to 172% of the matched control value (mean
= 136%). By contrast, there were no differences in the concentrations of neuron-specific
enolase protein in the same set of samples. Similarly, the number of neuromelanin-containing
cells, counted in sections of locus coeruleus adjacent to those taken for blot
immunolabeling analyses, did not differ between the two groups. These data indicate
that locus coeruleus neurons from suicide victims contain higher than normal concentrations
of tyrosine hydroxylase, thus raising the possibility that the expression of tyrosine
hydroxylase in locus coeruleus may be relevant in the pathophysiology of suicide."
[Abstract] Brady
LS, Whitfield HJ Jr, Fox RJ, Gold PW, Herkenham M.
Long-term antidepressant
administration alters corticotropin-releasing hormone, tyrosine hydroxylase, and
mineralocorticoid receptor gene expression in rat brain. Therapeutic implications.
J Clin Invest. 1991 Mar;87(3):831-7.
"Imipramine is the prototypic tricyclic
antidepressant utilized in the treatment of major depression and exerts its therapeutic
efficacy only after prolonged administration. We report a study of the effects
of short-term (2 wk) and long-term (8 wk) administration of imipramine on the
expression of central nervous system genes among those thought to be dysregulated
in imipramine-responsive major depression. As assessed by in situ hybridization,
8 wk of daily imipramine treatment (5 mg/kg, i.p.) in rats decreased corticotropin-releasing
hormone (CRH) mRNA levels by 37% in the paraventricular nucleus (PVN) of the hypothalamus
and decreased tyrosine hydroxylase (TH) mRNA levels by 40% in the locus coeruleus
(LC). These changes were associated with a 70% increase in mRNA levels of the
hippocampal mineralocorticoid receptor (MR, type I) that is thought to play an
important role in mediating the negative feedback effects of low levels of steroids
on the hypothalamic-pituitary-adrenal (HPA) axis. Imipramine also decreased proopiomelanocortin
(POMC) mRNA levels by 38% and glucocorticoid receptor (GR, type II) mRNA levels
by 51% in the anterior pituitary. With the exception of a 20% decrease in TH mRNA
in the LC after 2 wk of imipramine administration, none of these changes in gene
expression were evident as a consequence of short-term administration of the drug.
In the light of data that major depression is associated with an activation of
brain CRH and LC-NE systems, the time-dependent effect of long-term imipramine
administration on decreasing the gene expression of CRH in the hypothalamus and
TH in the LC may be relevant to the therapeutic efficacy of this agent in depression."
[Abstract] EJ
Nestler, A McMahon, EL Sabban, JF Tallman, and RS Duman
Chronic
Antidepressant Administration Decreases the Expression of Tyrosine Hydroxylase
in the Rat Locus Coeruleus
PNAS 87: 7522-7526, 1990.
"Regulation
of tyrosine hydroxylase expression by antidepressant treatments was investigated
in the locus coeruleus (LC), the major noradrenergic nucleus in brain. Rats were
treated chronically with various antidepressants, and tyrosine hydroxylase levels
were measured in the LC by immunoblot analysis. Representatives of all major classes
of antidepressant medication-including imipramine, nortriptyline, tranylcypromine,
fluvoxamine, fluoxetine, bupropion, iprindole, and electroconvulsive seizures-were
found to decrease levels of tyrosine hydroxylase immunoreactivity by 40-70% in
the LC. Decreased levels of enzyme immunoreactivity were shown to be associated
with equivalent decreases in enzyme mRNA levels. Antidepressant regulation of
LC tyrosine hydroxylase appeared specific to these compounds, inasmuch as chronic
treatment of rats with representatives of other classes of psychotropic drugs,
including haloperidol, diazepam, clonidine, cocaine, and morphine, failed to decrease
levels of this protein. The results demonstrate that chronic antidepressants dramatically
downregulate the expression of tyrosine hydroxylase in the LC and raise the possibility
that such regulation of the enzyme represents an adaptive response of LC neurons
to antidepressants that mediates some of their therapeutic actions in depression
and/or other psychiatric disturbances." [Abstract] Melia
KR, Nestler EJ, Duman RS.
Chronic imipramine treatment normalizes
levels of tyrosine hydroxylase in the locus coeruleus of chronically stressed
rats.
Psychopharmacology (Berl). 1992;108(1-2):23-6.
"Previous
studies have demonstrated that chronic stress increases and antidepressant treatments
decrease levels of tyrosine hydroxylase (TH) in locus coeruleus (LC). In the present
study, the influence of chronic antidepressant treatment on the induction of TH
immunoreactivity in response to cold stress is examined. It was found that chronic
imipramine pretreatment (18 days) attenuated the induction of TH in response to
cold stress, resulting in levels of TH immunoreactivity not different from control.
In contrast, imipramine pretreatment for 1 or 7 days was not sufficient to normalize
the stress-induced elevation of TH immunoreactivity. These findings raise the
possibility that the therapeutic action of antidepressants may be derived, in
part, from the ability of these treatments to normalize levels of TH and thereby
the function of the NE neurotransmitter system under conditions of stress."
[Abstract] Butterweck
V, Winterhoff H, Herkenham M.
Hyperforin-Containing Extracts of St
John's Wort Fail to Alter Gene Transcription in Brain Areas Involved in HPA Axis
Control in a Long-Term Treatment Regimen in Rats.
Neuropsychopharmacology.
2003 Jul 16 [Epub ahead of print].
"Fluoxetine (10 mg/kg) given daily
for 8 weeks, but not 2 weeks, significantly decreased levels of corticotropin-releasing
hormone (CRH) mRNA by 22% in the paraventricular nucleus (PVN) of the hypothalamus
and tyrosine hydroxylase (TH) mRNA by 23% in the locus coeruleus. Fluoxetine increased
levels of mineralocorticoid (MR) (17%), glucocorticoid (GR) (18%), and 5-HT(1A)
receptor (21%) mRNAs in the hippocampus at 8, but not 2, weeks." [Abstract] Zeng
J, Kitayama I, Yoshizato H, Zhang K, Okazaki Y.
Increased expression
of corticotropin-releasing factor receptor mRNA in the locus coeruleus of stress-induced
rat model of depression.
Life Sci. 2003 Jul 18;73(9):1131-9.
"Hypersecretion
of corticotropin-releasing factor (CRF) has been hypothesized to occur in depression.
To investigate CRF receptor (CRFR) response to the increased production of CRF
in chronically stressed rats, we measured by in situ hybridization the expression
of CRFR mRNA in the locus coeruleus (LC) concomitant with measuring plasma adrenocorticotropin
(ACTH). The expression of both CRFR mRNA in the LC and the plasma level of ACTH
increased significantly in "depression-model rats" which exhibit reduced
activity following exposure to 14 days forced walking stress (FWS), but not in
"spontaneous recovery rats" whose activity was restored after the long-term
stress. These results suggest that the LC neurons continue to be stimulated by
CRF, and that the hypothalamic-pituitary-adrenal (HPA) axis is hyperfunctioning
in the depression-model rats." [Abstract] Jezova
D, Ochedalski T, Glickman M, Kiss A, Aguilera G.
Central corticotropin-releasing
hormone receptors modulate hypothalamic-pituitary-adrenocortical and sympathoadrenal
activity during stress.
Neuroscience. 1999;94(3):797-802.
"The
role of brain corticotropin-releasing hormone receptors in modulating hypothalamic-pituitary-adrenal
and sympathoadrenal responses to acute immobilization stress was studied in conscious
rats under central corticotropin-releasing hormone receptor blockade by intracerebroventricular
injection of a peptide corticotropin-releasing hormone receptor antagonist. Blood
for catecholamines, adrenocorticotropic hormone and corticosterone levels was
collected through vascular catheters, and brains were removed at 3 h for in situ
hybridization for tyrosine hydroxylase messenger RNA in the locus coeruleus, and
corticotropin-releasing hormone and corticotropin-releasing hormone receptor messenger
RNA in the hypothalamic paraventricular nucleus. Central corticotropin-releasing
hormone receptor blockade reduced the early increases in plasma epinephrine and
dopamine, but not norepinephrine, during stress. Immobilization stress increased
tyrosine hydroxylase messenger RNA levels in the locus coeruleus by 36% in controls,
but not in corticotropin-releasing hormone antagonist-injected rats. In control
rats, corticotropin-releasing hormone messenger RNA and type 1 corticotropin-releasing
hormone receptor messenger RNA in the paraventricular nucleus increased after
stress (P<0.01), and these responses were attenuated by central corticotropin-releasing
hormone receptor blockade. In contrast, central corticotropin-releasing hormone
antagonist potentiated plasma adrenocorticotropic hormone responses, but slightly
attenuated plasma corticosterone responses to stress. The inhibition of plasma
catecholamine and locus coeruleus tyrosine hydroxylase messenger RNA responses
to stress by central corticotropin-releasing hormone receptor blockade supports
the notion that central corticotropin-releasing hormone regulates sympathoadrenal
responses during stress. The attenuation of stress-induced corticotropin-releasing
hormone and corticotropin-releasing hormone receptor messenger RNA responses by
central corticotropin-releasing hormone receptor blockade suggests direct or indirect
positive feedback effects of corticotropin-releasing hormone receptor ligands
on corticotropin-releasing hormone expression, whereas additional mechanisms potentiate
adrenocorticotropic hormone responses at the pituitary level. In addition, changes
in neural activity by central corticotropin-releasing hormone are likely to modulate
adrenocortical responsiveness during stress." [Abstract]
Roy
A, Pickar D, Linnoila M, Chrousos GP, Gold PW.
Cerebrospinal fluid
corticotropin-releasing hormone in depression: relationship to noradrenergic function.
Psychiatry Res 1987 Mar;20(3):229-37
"We investigated the neurotransmitter
regulation of corticotropin-releasing hormone (CRH). Among 21 depressed patients
cerebrospinal fluid (CSF) levels of CRH significantly correlated with urinary
outputs of norepinephrine and its major metabolites, and there were trends for
significant correlations with both CSF and plasma levels of norepinephrine. These
results suggest that CRH may be associated with the dysregulation of the norepinephrine
system that is found in [depression]." [Abstract]
Arborelius
L, Owens MJ, Plotsky PM, Nemeroff CB.
The role of corticotropin-releasing
factor in depression and anxiety disorders.
J Endocrinol
1999 Jan;160(1):1-12
"In the present review, we describe the evidence
suggesting that CRF is hypersecreted from hypothalamic as well as from extrahypothalamic
neurons in depression, resulting in hyperactivity of the hypothalamic-pituitary-adrenal
(HPA) axis and elevations of cerebrospinal fluid (CSF) concentrations of CRF.
This increase in CRF neuronal activity is also believed to mediate certain of
the behavioral symptoms of depression involving sleep and appetite disturbances,
reduced libido, and psychomotor changes. The hyperactivity of CRF neuronal systems
appears to be a state marker for depression because HPA axis hyperactivity normalizes
following successful antidepressant treatment. Similar biochemical and behavioral
findings have been observed in adult rats and monkeys that have been subjected
to early-life stress. In contrast, clinical studies have not revealed any consistent
changes in CSF CRF concentrations in patients with anxiety disorders; however,
preclinical findings strongly implicate a role for CRF in the pathophysiology
of certain anxiety disorders, probably through its effects on central noradrenergic
systems. The findings reviewed here support the hypothesis that CRF receptor antagonists
may represent a novel class of antidepressants and/or anxiolytics." [Abstract] Banki
CM, Bissette G, Arato M, O'Connor L, Nemeroff CB.
CSF corticotropin-releasing
factor-like immunoreactivity in depression and schizophrenia.
Am J Psychiatry 1987 Jul;144(7):873-7
"To further investigate the hypothesis
that hyperactivity of the hypothalamic-pituitary-adrenal axis in patients with
depression may be mediated by hypersecretion of corticotropin-releasing factor
(CRF), the authors measured CRF-like immunoreactivity in CSF samples from 138
neurological control, 54 depressed, and 27 nondepressed (23 schizophrenic and
four manic) subjects. The CSF CRF concentration was markedly higher (almost twofold)
in depressed patients than in control subjects and nondepressed psychiatric patients.
The concentration of CSF CRF was slightly but significantly higher in schizophrenic
patients than in control subjects. These findings provide further support for
the hypothesis that CRF hypersecretion occurs in major depression." [Abstract] Schulz
C, Lehnert H.
Activation of noradrenergic neurons in the locus coeruleus
by corticotropin-releasing factor. A microdialysis study.
Neuroendocrinology 1996 May;63(5):454-8
"In the present study the effects
of different doses of corticotropin-releasing factor (CRF) and the CRF antagonist
alpha-helical CRF on locus coeruleus (LC) neurons were studied in anesthetized
male Wistar rats. To monitor the release of noradrenaline (NA) and its metabolite
3-methoxy-4-hydroxyphenylethylene glycol (MHPG), a microdialysis probe was implanted
into the parietal cortex, a major projection area of the LC. Saline, 0.17, 0.51
nmol CRF and a combination of 5.1 nmol alpha-helical CRF and 0.51 nmol CRF were
applied to the LC via a fused silica capillary. While both doses of CRF augmented
NA in parietal cortex dialysates (0.51 nmol CRF: from 0.0206 to 0.0266 pmol/sample;
0.17 nmol CRF: from 0.0147 to 0.0170 pmol/sample), saline did not affect NA concentration.
The metabolite MHPG also increased, but in a more prolonged time course. The antagonist
alpha-helical CRF attenuated the CRF effects. The increase of extraneuronal NA
concentration monitored in the cortical samples indicates an augmented depolarization
rate of noradrenergic LC neurons. This clearly demonstrates the activation of
these neurons by CRF, suggesting physiological interactions of CRF and noradrenergic
neurons." [Abstract] Emoto
H, Tanaka M, Koga C, Yokoo H, Tsuda A, Yoshida M.
Corticotropin-releasing
factor activates the noradrenergic neuron system in the rat brain.
Pharmacol Biochem Behav 1993 Jun;45(2):419-22
"The effect of corticotropin-releasing
factor (CRF) on central noradrenaline (NA) metabolism was examined by measuring
levels of the major metabolite of NA, 3-methoxy-4-hydroxy-phenylethyleneglycol
sulfate (MHPG-SO4) in several rat brain regions. Various doses of CRF ranging
from 0.5-10 micrograms injected ICV significantly increased MHPG-SO4 levels in
several brain regions including the hypothalamus, amygdala, midbrain, locus coeruleus
(LC) region, and pons + medulla oblongata excluding the LC region. Plasma corticosterone
levels were also significantly increased after ICV CRF administration up to 0.5
micrograms. The present results that CRF not only elevates plasma corticosterone
levels but also increases NA metabolism in many brain regions suggest its neurotransmitter
and/or neuromodulator role exerting the excitatory action on central NA neurons."
[Abstract]
Emoto H, Koga C, Ishii H, Yokoo H, Yoshida M, Tanaka M.
A CRF antagonist attenuates stress-induced increases in NA turnover
in extended brain regions in rats.
Brain Res 1993 Nov 5;627(1):171-6
"We investigated the effects of intracerebroventricular (i.c.v.) administration
of corticotropin-releasing factor (CRF) antagonist, alpha-helical CRF9-41 (ahCRF),
on increases in noradrenaline (NA) turnover caused by immobilization stress in
rat brain regions. Pretreatment with ahCRF (50 or 100 micrograms) significantly
attenuated increases in levels of 3-methoxy-4-hydroxyphenylethyleneglycol sulfate
(MHPG-SO4), the major metabolite of NA in rat brain, in the locus coeruleus (LC)
region, and attenuated the MHPG-SO4/NA ratio after immobilization stress for 50
min in the cerebral cortex, hippocampus, amygdala, midbrain and hypothalamus.
However, stress-induced increases in plasma corticosterone levels were not decreased
significantly by pretreatment with ahCRF. These results suggest that CRF, released
during stress, causes increases in NA release in extended brain regions of stressed
rats." [Abstract] Valentino
RJ, Foote SL, Page ME.
The locus coeruleus as a site for integrating
corticotropin-releasing factor and noradrenergic mediation of stress responses.
Ann N Y Acad Sci 1993 Oct 29;697:173-88
"It could be predicted that the
effects of CRF neurotransmission in the LC during stress would enhance information
processing concerning the stressor or stimuli related to the stressor by LC target
neurons. One consequence of this appears to be increased arousal. Although this
may be adaptive in the response to an acute challenge, it could be predicted that
chronic CRF release in the LC would result in persistently elevated LC discharge
and norepinephrine release in targets. This could be associated with hyperarousal
and loss of selective attention as occurs in certain psychiatric diseases. Manipulation
of endogenous CRF systems may be a novel way in which to treat psychiatric diseases
characterized by these maladaptive effects." [Abstract] Curtis
AL, Valentino RJ.
Corticotropin-releasing factor neurotransmission
in locus coeruleus: a possible site of antidepressant action.
Brain Res Bull 1994;35(5-6):581-7
"Hypersecretion of corticotropin-releasing
factor (CRF), has been hypothesized to occur in depression. Because CRF may serve
as a neurotransmitter in the locus coeruleus (LC), it was proposed that CRF hypersecretion
in the LC is responsible for some characteristics of depression, and that antidepressants
act by interfering with CRF neurotransmission in the LC. To test this hypothesis,
the acute and chronic effects of four antidepressants and cocaine were characterized
on LC spontaneous and sensory-evoked discharge, LC activation by a stressor that
requires CRF release, and LC activation by exogenously administered CRF. None
of the antidepressants or cocaine altered LC activation by intracerebroventricularly
administered CRF (3.0 microgram) after chronic administration. However, chronic
administration of desmethylimipramine and mianserin inhibited LC activation by
a hypotensive stress that requires endogenous CRF release, suggesting that they
decrease CRF release in the LC. Chronic administration of sertraline and phenelzine
altered LC responses to repeated sciatic nerve stimulation in a manner opposite
to the effect produced by CRF, suggesting that these drugs may functionally antagonize
CRF actions in the LC. Cocaine did not appear to interfere with CRF actions in
the LC. In conclusion, chronic administration of antidepressants may have the
potential to interfere with CRF neurotransmission in the LC." [Abstract] Valentino
RJ, Curtis AL.
Pharmacology of locus coeruleus spontaneous and
sensory-evoked activity.
Prog Brain Res 1991;88:249-56
"Neuroendocrine and catecholamine dysfunctions in depression may be linked
by corticotropin-releasing factor (CRF) effects on locus coeruleus (LC) neurons.
One consequence of CRF hypersecretion in depression would be persistent elevated
levels of LC discharge and diminished responses to phasic sensory stimuli. The
hypothesis that antidepressants could reverse these changes was tested by characterizing
effects of pharmacologically distinct antidepressants on LC sensory-evoked discharge,
LC activation by stress, and LC activation by CRF. The most consistent effect
of all of the antidepressants tested was a decrease in LC sensory-evoked discharge
after acute administration. However, tolerance occurs to these effects after chronic
administration. With chronic administration each of the antidepressants produced
effects which could potentially interfere with CRF function in the LC. Desmethylimipramine
and mianserin attenuated LC activation by a stressor which requires endogenous
CRF, suggesting that these antidepressants attenuate stress-elicited release of
CRF and perhaps the hypersecretion that occurs in depression. The serotonin reuptake
inhibitor, sertraline (SER), enhanced the signal-to-noise ratio of the LC sensory
response, an effect opposite to that of CRF. Thus, SER could serve as a functional
antagonist of CRF that is hypersecreted in depression. The finding that three
pharmacologically distinct antidepressants share the potential to interfere with
CRF function in the LC implies that this may be an important common mechanism
for antidepressant activity." [Abstract] Curtis,
Andre L., Pavcovich, Luis A., Valentino, Rita J.
Long-Term Regulation
of Locus Ceruleus Sensitivity to Corticotropin-Releasing Factor by Swim Stress
J Pharmacol Exp Ther 1999 289: 1211-1219
"Corticotropin-releasing factor
(CRF) acts as a putative neurotransmitter in the locus ceruleus (LC) to mediate
its activation by certain stressors. In this study, we quantified LC sensitivity
to CRF 24 h after swim stress, at a time when behavioral depression that is sensitive
to antidepressants is apparent. Rats were placed in a tank with 30 cm (swim stress)
or 4 cm water and 24 h later, either behavior was monitored in a forced swim test
or LC discharge was recorded. Swim stress rats were more immobile than control
animals in the swim test. LC neurons of swim stress rats were sensitized to low
doses of CRF (0.1-0.3 µg i.c.v.) that were ineffective in control animals
and were desensitized to higher doses. Swim stress selectively altered LC sensitivity
to CRF because neither LC spontaneous discharge nor responses to other agents
(e.g., carbachol, vasoactive intestinal peptide) were altered. Finally, the mechanism
for sensitization was localized to the LC because neuronal activation by low doses
of CRF was prevented by the intracerulear administration of a CRF antagonist.
CRF dose-response curves were consistent with a two-site model with similar dissociation
constants under control conditions but divergent dissociation constants after
swim stress. The results suggest that swim stress (and perhaps other stressors)
functionally alters CRF receptors that have an impact on LC activity. Stress-induced
regulation of LC sensitivity to CRF may underlie behavioral aspects of stress-related
psychiatric disorders." [Full
Text] Van Bockstaele EJ, Colago EE, Valentino
RJ.
Corticotropin-releasing factor-containing axon terminals synapse
onto catecholamine dendrites and may presynaptically modulate other afferents
in the rostral pole of the nucleus locus coeruleus in the rat brain.
J Comp Neurol 1996 Jan 15;364(3):523-534 [Abstract]
Smagin GN, Swiergiel AH, Dunn AJ.
Corticotropin-releasing
factor administered into the locus coeruleus, but not the parabrachial nucleus,
stimulates norepinephrine release in the prefrontal cortex.
Brain Res Bull 1995;36(1):71-6 [Abstract] Lamberts
SW, Bons E, Zuiderwijk J.
High concentrations of catecholamines selectively
diminish the sensitivity of CRF-stimulated ACTH release by cultured rat pituitary
cells to the suppressive effects of dexamethasone.
Life
Sci 1986 Jul 14;39(2):97-102
"ACTH-release by primary cultures of rat
anterior pituitary cells in response to CRF, vasopressin, epinephrine, norepinephrine
and VIP is readily suppressible by dexamethasone. Rat hypothalamic extract-induced
ACTH release is less sensitive to the inhibitory effect of dexamethasone than
that elicited by CRF and the other secretagogues mentioned above. In studying
the additive and potentiating effect on ACTH release of CRF in combination with
vasopressin, VIP and the catecholamines it became evident that only the combination
of micromolar concentrations of epinephrine or norepinephrine together with nanomolar
concentrations of CRF will make ACTH release significantly less sensitive to the
suppressive effect of dexamethasone. Other combinations of CRF and vasopressin
or CRF and VIP will render ACTH release as suppressible to dexamethasone, as that
elicited by each of these compounds by itself. This observation in the rat might
explain at least in part the observation that a diminished suppressibility of
the pituitary-adrenal axis to dexamethasone can be found in patients with psychiatric
disease, especially depression." [Abstract]
Maes M, Vandewoude M, Schotte C, Martin M, Blockx
P.
Positive relationship between the catecholaminergic turnover and
the DST results in depression.
Psychol Med. 1990 Aug;20(3):493-9.
"In
the past some workers have reported positive relationships between indices of
noradrenaline activity and measures of hypothalamic-pituitary-adrenal (HPA)-axis
function. In order to investigate these relations, the authors measured noradrenaline,
adrenaline and vanillylmandelic acid (VMA) in 24 h urine samples of 72 depressed
females. Serum adrenocorticotrophic hormone (ACTH) and cortisol concentrations
were determined before and after administration of 1 mg of dexamethasone. Cortisol
non-suppressors exhibited a significantly higher noradrenaline, adrenaline and
VMA excretion as compared to cortisol suppressors. We determined significantly
positive correlations between the postdexamethasone cortisol values and the excretion
rates of noradrenaline and VMA. These indices of noradrenaline activity correlated
neither with the baseline cortisol and ACTH nor with the postdexamethasone ACTH
values." [Abstract] Roy
A, Pickar D, De Jong J, Karoum F, Linnoila M.
Norepinephrine and
its metabolites in cerebrospinal fluid, plasma, and urine. Relationship to hypothalamic-pituitary-adrenal
axis function in depression.
Arch Gen Psychiatry 1988 Sep;45(9):849-57
"Among 140 depressed and control subjects, there were significant positive
correlations between indexes of noradrenergic activity in cerebrospinal fluid
(CSF), plasma, and urine. Among the depressed patients, CSF levels of the norepinephrine
(NE) metabolite 3-methoxy-4-hydroxyphenylglycol (MHPG) and urinary outputs of
NE and its metabolites normetanephrine, MHPG, and vanillylmandelic acid correlated
significantly with plasma cortisol levels in relation to dexamethasone administration.
Also, CSF levels of MHPG were significantly higher among patients who were cortisol
nonsuppressors than among either patients who were cortisol suppressors or controls.
Urinary outputs of NE and normetanephrine were significantly higher among patients
who were cortisol nonsuppressors than among controls. Patients who were cortisol
suppressors had indexes of NE metabolism similar to those of controls. These results
in the depressed patients extend recent observations suggesting that dysregulation
of the noradrenergic system and hypothalamic-pituitary-adrenal axis occur together
in a subgroup of depressed patients." [Abstract] Golczynska
A, Lenders JW, Goldstein DS.
Glucocorticoid-induced sympathoinhibition
in humans.
Clin Pharmacol Ther. 1995 Jul;58(1):90-8.
"OBJECTIVE:
To test whether glucocorticoids inhibit sympathetic nerve activity or norepinephrine
release in humans, as has been suggested by results in laboratory animals. METHODS:
This was a double-blind, placebo-controlled, randomized crossover study performed
at the Clinical Center of the National Institutes of Health. Thirteen normal volunteers
received 20 mg prednisone or placebo orally each morning for 1 week, followed
by a washout period of 1 week and then by treatment with the other drug for 1
week. On the last day of each treatment week, blood samples were drawn for measurements
of plasma levels of catecholamines and their metabolites, of cortisol, and of
corticotropin at baseline and during reflexive sympathetic stimulation elicited
by lower body negative pressure (-15 mm Hg). A 24-hour urine collection was obtained
at the end of each week of treatment for measurement of urinary excretion of catechols.
In eight subjects, directly recorded peroneal skeletal muscle sympathetic nerve
activity was also measured after both treatments. RESULTS: Prednisone significantly
decreased sympathetic nerve activity by 23% +/- 6%, plasma norepinephrine levels
by 27% +/- 6%, and plasma corticotropin levels by 77%. Blood pressure, heart rate,
body weight, and urinary excretion of catechols and electrolytes were unaffected.
Prednisone did not alter proportionate increments in sympathetic nerve activity
or plasma norepinephrine levels during lower body negative pressure. Relationships
between sympathetic nerve activity and plasma norepinephrine levels were unchanged.
CONCLUSIONS: Glucocorticoids decrease sympathoneural outflows in humans without
affecting acute sympathoneural responses to decreased cardiac filling and probably
without affecting presynaptic modulation of norepinephrine release." [Abstract] Raucoules
D, Levy C, Azorin JM, Bruno M, Valli M.
[Plasma levels of MHPG,
HVA and total 5-HIAA in depression. Preliminary study]
Encephale 1992 Nov-Dec;18(6):611-6
"This study was aimed at assessing
monoamine catabolites plasma levels in depressed patients and healthy volunteers.
Plasma levels of 3-methoxy-4-hydroxyphenylglycol (MHPG), homovanillic acid (HVA),
and 5-hydroxyindoleacetic acid (5-HIAA) of 21 control subjects and 26 depressed
patients (according to DSM III-R criteria) were measured at baseline (day 0) and
day 4, day 7, day 30 of prescribed antidepressant treatment. The clinical assessment,
at baseline as well as during treatment, used the Hamilton depression rating scale
and the BPRS. Our data show the interest of these results in predicting response.
The respondent patients showed a significant decrease in plasma MHPG level at
J7, contrary to non-respondent patients. Moreover, a positive correlation between
plasma levels of MHPG and HVA before any prescribed antidepressants was found
only with respondent patients. The lack of correlation for non-respondent patients
can suggest that the relationships between this monoamine systems should be disrupted
in these patients." [Abstract] Schildkraut
JJ, Orsulak PJ, LaBrie RA, Schatzberg AF, Gudeman JE, Cole JO, Rohde WA.
Toward
a biochemical classification of depressive disorders. II. Application of multivariate
discriminant function analysis to data on urinary catecholamines and metabolites.
Arch Gen Psychiatry 1978 Dec;35(12):1436-9
"The previous article in this
series reported on the differences in urinary excretion of 3-methoxy-4-hydroxyphenylglycol
(MHPG) in patients with various clinically defined subtypes of depressive disorders.
We now report that further biochemical discrimination among depressive subtypes
is provided by the following equation, derived empirically by applying multivariate
discriminant function analysis to data on urinary catecholamine metabolits: Depression-type
(D-type) score = C1(MHPG) + C2(VMA) + C3(NE) +C4(NMN + MN)/VMA + C0. In the original
derivation of this equation, low scores were related to bipolar manic-depressive
depressions, and high scores were related to unipolar nonendogenous (chronic characterological)
depressions. Findings from a series of depressed patients whose biochemical data
had not been used to derive this equation confirmed these differences in D-type
scores among subtypes of depressions. The findings presented in this report further
suggest that we can discriminate three biochemically discrete subgroups of depressive
disorders." [Abstract] Roy
A, Pickar D, Douillet P, Karoum F, Linnoila M.
Urinary monoamines
and monoamine metabolites in subtypes of unipolar depressive disorder and normal
controls.
Psychol Med 1986 Aug;16(3):541-6
"An
examination was made of urinary catecholamine and metabolite outputs in 28 unipolar
depressed patients and 25 normal controls. The total group of depressed patients
had significantly higher urinary outputs of norepinephrine (NE) and its metabolite
normetanephrine (NM), and significantly lower urinary outputs of the dopamine
metabolite dihydroxyphenylacetic acid (DOPAC), than controls. Patients who met
DSM-III criteria for a major depressive episode with melancholia (N = 8) had significantly
higher urinary outputs of normetanephrine than controls, whereas patients with
a major depressive episode without melancholia (N = 7) and dysthymic disorder
patients (N = 8) had levels comparable with controls. We postulate that the higher
urinary outputs of norepinephrine and its metabolite, normetanephrine, reflect
dysregulation of the sympathetic nervous system in depression." [Abstract] Roy
A, Linnoila M, Karoum F, Pickar D.
Relative activity of metabolic
pathways for norepinephrine in endogenous depression.
Acta
Psychiatr Scand 1986 Jun;73(6):624-8
"Thirteen patients with endogenous
depression, compared to 25 normal controls, had a significantly greater ratio
of the urinary excretion of norepinephrine plus its metabolite normetanephrine
to either the sum of the two urinary norepinephrine metabolites 3-methoxy-4-hydroxyphenylglycol
plus vanillylmandelic acid or to the sum of urinary norepinephrine and all of
its metabolites. As urinary levels of norepinephrine and normetanephrine are derived
from an extraneuronal metabolic pathway, while levels of 3-methoxy-4-hydroxyphenylglycol
and vanillylmandelic acid are more representative of total norepinephrine metabolism,
these results suggest that there is a shift in endogenous depression to extraneuronal
metabolic pathways for norepinephrine and its metabolites." [Abstract] Beckmann
H, Goodwin FK.
Urinary MHPG in subgroups of depressed patients
and normal controls.
Neuropsychobiology 1980;6(2):91-100
"3-Methoxy-4-hydroxyphenylglycol (MHPG), the urinary metabolite thought best
to reflect brain norepinephrine metabolism, was studied in a large group of hospitalized
depressed patients with primary affective disorder and in normal controls, as
part of an ongoing effort to evaluate the role of central amine dysfunction in
affective illness. Overall there was no difference in MHPG between the depressed
patients and controls. Hosever, within the depressed population the bipolar patients
excreted significantly less MHPG than the unipolars and, as a group, the male
bipolar patients had significantly lower MHPG than male controls. MHPG correlated
positively with age, age of onset, rating of anxiety and psychosis and, most importantly,
with systolic blood pressure. These data support the concept of biological heterogeneity
among individuals with major depressive disorders. However, the relationship between
MHPG excretion and various psychological and physiological parameters is both
intriguing and complex and warrants careful interpretation." [Abstract] Roy
A, Pickar D, Linnoila M, Doran AR, Ninan P, Paul SM.
Cerebrospinal
fluid monoamine and monoamine metabolite concentrations in melancholia.
Psychiatry
Res 1985 Aug;15(4):281-92
"Cerebrospinal fluid levels of norepinephrine
and six monoamine metabolites were measured in 28 medication-free depressed patients.
Patients with a major depressive episode with melancholia (n = 15) had significantly
lower levels of the three dopamine metabolites: homovanillic acid (HVA), dihydroxyphenylacetic
acid (DOPAC), and conjugated dihydroxyphenylacetic (CONJDOPAC), when compared
with a combined group of patients with a major depressive episode or dysthymic
disorder (n = 13). In patients with major depressive episode with melancholia,
levels of HVA and of the serotonin metabolite 5-hydroxyindoleacetic acid significantly
correlated with the severity of depression. In the total group of 28 depressed
patients, cerebrospinal fluid (CSF) levels of norepinephrine significantly correlated
with symptoms of anxiety. In both patients with major depressive episode and major
depressive episode with melancholia, those who were non-suppressors on the dexamethasone
suppression test had significantly higher CSF levels of the norepinephrine metabolite
3-methoxy-4-hydroxyphenylglycol compared to those who were suppressors."
[Abstract] Yazici
O, Aricioglu F, Gurvit G, Ucok A, Tastaban Y, Canberk O, Ozguroglu M, Durat T,
Sahin D.
Noradrenergic and serotoninergic depression?
J Affect Disord 1993 Feb;27(2):123-9
"The only significant finding in
this study was the obvious decrease in MHPG excretion during the antidepressant
treatment in the group with high pretreatment MHPG." [Abstract] Potter
WZ, Manji HK.
Catecholamines in depression: an update.
Clin Chem 1994 Feb;40(2):279-87
"Despite extensive research, the biochemical
abnormalities underlying the predisposition to and the pathogenesis of affective
disorders remain to be clearly established. Efforts to study norepinephrine (NE)
output and function have utilized biochemical assays, neuroendocrine challenge
strategies, and measures of peripheral blood cell receptors; the cumulative database
points to a dysregulation of the noradrenergic system. Depressed patients (in
particular, melancholic, unipolar subjects) excrete disproportionately greater
amounts of NE and its major extraneuronal metabolite, normetanephrine, than do
controls. Depressed patients also show subsensitive neuroendocrine (growth hormone)
and biochemical (inhibition of adenylate cyclase) responses to alpha 2-adrenergic
agonists, suggesting that subsensitivity of nerve terminal alpha 2 autoreceptors
may underlie the exaggerated plasma NE observed in response to various challenges
in affective disorders. Future advances in brain imaging techniques and in the
molecular biology of adrenergic receptor-coupled signal transduction systems offer
promise for meaningful advances in our understanding of the pathophysiology of
affective disorders." [Abstract] Backman
J, Alling C, Alsen M, Regnell G, Traskman-Bendz L.
Changes of cerebrospinal
fluid monoamine metabolites during long-term antidepressant treatment.
Eur Neuropsychopharmacol 2000 Sep;10(5):341-9
"This study describes the
changes in cerebrospinal fluid (CSF) monoamine metabolites during antidepressant
treatment for more than 6 months. Eight patients, who received antidepressant
treatment after attempted suicide and then underwent lumbar punctures every 3
or 4 months, were included. Plasma drug concentrations and the clinical outcome
were also measured. Consistent with previous reports about antidepressant treatment
for between 3 and 6 weeks, both 3-methoxy-4-hydroxyphenylethyleneglycol (MHPG)
and 5-hydroxyindoleacetic acid (5-HIAA) were significantly decreased after treatment
for a mean of 15 weeks compared to pretreatment. However, after continued treatment
for a mean of 30 weeks the MHPG concentration remained significantly lower than
at pretreatment while 5-HIAA had returned to the pretreatment level. The clinical
outcome was significantly correlated to the pretreatment 5-HIAA/MHPG ratio. These
results suggest that the frequently reported reduction in CSF 5-HIAA after antidepressant
treatment does not remain during long-term treatment." [Abstract] Mine
K, Okada M, Mishima N, Fujiwara M, Nakagawa T.
Plasma-free and sulfoconjugated
MHPG in major depressive disorders: differences between responders to treatment
and nonresponders.
Biol Psychiatry 1993 Nov 1;34(9):654-60
"The plasma levels of free and sulfoconjugated forms of 3-methoxy-4-hydroxyphenylglycol
(MHPG) were examined before and after treatment in 16 patients with unipolar major
depressive disorders without melancholia. The patients were treated with intravenous
administration of clomipramine for 4 weeks. Seven depressive disorder patients
who showed marked improvement (the improvement group) revealed significant reduction
in their plasma sulfoconjugated MHPG levels. In 6 depressive disorder patients
who showed no improvement (the no-improvement group), the plasma sulfoconjugated
MHPG levels showed no significant change after treatment. The remaining 3 patients,
who showed ambiguous change after treatment, were excluded from the analysis.
Levels of plasma-free MHPG showed significant change after treatment in neither
the improvement group nor in the no-improvement group. It is suggested that levels
of plasma sulfoconjugated MHPG may serve as an indicator of brain noradrenergic
activity." [Abstract] Karege
F, Bovier P, Hilleret H, Gaillard JM.
Lack of effect of anxiety
on total plasma MHPG in depressed patients.
J Affect Disord
1993 Jul;28(3):211-7
"This report was undertaken to test the noradrenergic
deficiency hypothesis of depression and the postulated increase in noradrenergic
activity associated to anxiety states. A possible dual effect of both depression
and anxiety on total plasma MHPG levels was hypothesized and assessed in anxious
and non-anxious depressed patients. The findings show a decrease in plasma MHPG
levels in depressed patients whatever their degree of anxiety. There was no difference
in total plasma MHPG levels either between anxious and non-anxious depressed patients
or between low and high anxiety to depression ratio (ADR) depressed patients.
Following antidepressant drug-treatment, a decrease in plasma MHPG was found.
A positive correlation between the drug-induced decrease in NA activity and the
severity of depression was observed, and suggested a relationship between the
severity of depression and the instability of the NA system. No correlation between
the drug-induced decrease in plasma MHPG and the degree of anxiety was found.
The results do not suggest out an effect of anxiety on total plasma MHPG levels
in depressed patients." [Abstract] Correa
H, Duval F, Claude MM, Bailey P, Tremeau F, Diep TS, Crocq MA, Castro JO, Macher
JP.
Noradrenergic dysfunction and antidepressant treatment response.
Eur Neuropsychopharmacol 2001 Apr;11(2):163-8
"The purpose of this study
was to investigate differences in outcome following treatment with two different
antidepressants in depressed patients according to their pretreatment hormonal
response to clonidine. In all, 62 drug-free DSM-IV recurrent major depressed patients
and 20 normal controls were studied. Patients were subsequently treated for 4
weeks with fluoxetine (n=28), or amitriptyline (n=34), and were then classified
as responders or nonresponders according to their final Hamilton depression scale
score. Compared to controls, depressed patients showed lower GH response to CLO
(DeltaGH) (P<0.0002). One control (5%) and 35 depressed patients (56%) had
blunted DeltaGH values. The efficacy of the two antidepressants was not significantly
different: 15 patients responded to AMI (44%), seven patients responded to FLUOX
(25%) (P>0.15). However, in the subgroup of patients with blunted DeltaGH levels,
the rate of responders was higher for AMI (11/21) compared to FLUOX (1/14) treated
patients (P<0.01). These results suggest that in depressed patients a blunted
GH response to CLO could predict antidepressant response." [Abstract] Markianos
M, Alevizos B, Hatzimanolis J, Stefanis C.
Effects of monoamine
oxidase A inhibition on plasma biogenic amine metabolites in depressed patients.
Psychiatry Res 1994 Jun;52(3):259-64
"The main metabolites of noradrenalin,
dopamine, and serotonin-3-methoxy-4-hydroxyphenylglycol (MHPG), homovanillic acid
(HVA), and 5-hydroxyindoleacetic acid (5-HIAA), respectively--were estimated in
plasma of 21 depressed patients before and after 2 and 4 weeks of treatment with
the monoamine oxidase-type A (MAO-A) inhibitor moclobemide (mean final daily dose
= 8.9 mg/kg body weight). The treatment caused significant mean reductions in
plasma MHPG and HVA (46% and 30%, respectively), while plasma 5-HIAA was unchanged.
Multiple regression analysis revealed associations between reductions in MHPG
and changes on the anxiety-somatization factor of the Hamilton Rating Scale for
Depression (HRSD), and between reductions in HVA and changes in the HRSD factors
cognitive disturbance and retardation." [Abstract] |
Stout SC, Owens MJ, Nemeroff CB.
Regulation
of corticotropin-releasing factor neuronal systems and hypothalamic-pituitary-adrenal
axis activity by stress and chronic antidepressant treatment.
J Pharmacol Exp Ther 2002 Mar;300(3):1085-92
"In a series of experiments,
we tested the hypothesis that chronic antidepressant drug administration reduces
the synaptic availability of corticotropin-releasing factor (CRF) through one
or more effects on CRF gene expression or peptide synthesis. We also determined
whether effects of acute or chronic stress on CRF gene expression or peptide concentration
are influenced by antidepressant drug treatment. Four-week treatment with venlafaxine,
a dual serotonin (5-HT)/norepinephrine (NE) reuptake inhibitor, and tranylcypromine,
a monoamine oxidase inhibitor, resulted in an attenuation of acute stress-induced
increases in CRF heteronuclear RNA (hnRNA) synthesis in the paraventricular nucleus
(PVN). Trends toward the same effect were observed after treatment with the 5-HT
reuptake inhibitor fluoxetine, or the NE reuptake inhibitor reboxetine. CRF mRNA
accumulation in the PVN during exposure to chronic variable stress was attenuated
by concurrent antidepressant administration. Basal CRF hnRNA and mRNA expression
were not affected by antidepressant treatment in the PVN or in other brain regions
examined. Chronic stress reduced CRF concentrations in the median eminence, but
there were no consistent effects of antidepressant drug treatment on CRF, serum
corticotropin, or corticosterone concentrations. CRF receptor expression and basal
and stress-stimulated HPA axis activity were unchanged after antidepressant administration.
These results suggest that chronic antidepressant administration diminishes the
sensitivity of CRF neurons to stress rather than alters their basal activity.
Additional studies are required to elucidate the functional consequences and mechanisms
of this interaction." [Abstract]
Manier DH, Shelton RC, Sulser F.
Noradrenergic
antidepressants: does chronic treatment increase or decrease nuclear CREB-P?
J Neural Transm 2002;109(1):91-9
"Chronic administration of noradrenergic
antidepressants causes a desensitization of the beta adrenoceptor coupled adenylate
cyclase system." [Abstract]
Widmaier EP, Lim AT, Vale W.
Secretion of
corticotropin-releasing factor from cultured rat hypothalamic cells: effects of
catecholamines.
Endocrinology 1989 Feb;124(2):583-90
"An understanding of the regulation of CRF secretion in rats is currently
incomplete, in part due to the lack of sensitive in vitro models available for
studying this neuropeptide. In particular, the effects of catecholamines on CRF
secretion, and the receptor subtypes mediating these actions have long been the
subject of much debate. A cultured cell model has been adapted for studying secretory
responses of hypothalamic cells of 1-week-old rats. Between 7-16 days in monolayer
culture the cells secreted detectable levels of immunoreactive CRF, and this release
was paralleled by the appearance of punctate bead-like regions of immunoreactivity
along fine cellular processes. CRF secretion was increased up to 4-fold by norepinephrine
(EC50, approximately 0.5 microM). The increase in CRF secretion produced by norepinephrine
was blocked by the beta-receptor antagonist propranolol, but not by the alpha-antagonist
prazosin. Moreover, the beta-receptor agonist isoproterenol significantly elevated
CRF secretion, whereas the alpha-agonist phenylephrine was without effect, except
at high concentrations. Addition of phenylephrine, however, potentiated the effect
of isoproterenol, but this response was still significantly less than that produced
by norepinephrine. Forskolin (EC50, approximately 0.7 microM) and the active phorbol
ester 12-O-tetradecanoyl-phorbol-13-acetate (EC50, approximately 40 nM) also increased
CRF secretion by 3- to 4-fold. Inactive phorbol derivatives had no effect on CRF
release from these cultures. The results indicate that cultured neonatal rat hypothalamic
cells are a powerful model for the study of CRF release in vitro, and that norepinephrine
acts directly at the isolated cell level to stimulate secretion of this peptide,
primarily by activating beta-adrenoceptors. The results also suggest that at least
two functional second messenger systems (adenylate cyclase and protein kinase-C)
are involved in CRF secretion and are already functional in the neonatal hypothalamus."
[Abstract] Tilders
FJ, Berkenbosch F, Vermes I, Linton EA, Smelik PG.
Role of epinephrine
and vasopressin in the control of the pituitary-adrenal response to stress.
Fed Proc 1985 Jan;44(1 Pt 2):155-60
"In addition to corticotropin-releasing
factor (CRF) and structurally related peptides, arginine vasopressin (AVP), oxytocin,
angiotensin II, vasoactive intestinal polypeptide, peptide histidine isoleucinamide,
epinephrine (E), and norepinephrine induce secretion of adrenocorticotropin (ACTH)
from corticotropic cells in vitro. The apparent affinity and intrinsic ACTH-releasing
activity of these substances are lower than those of CRF. These substances can
also act synergistically with CRF. In this paper the role of catecholamines and
AVP in the control of ACTH release is discussed. Infusion i.v. of E increases
plasma ACTH and corticosterone to levels that are normally found during stress.
E-induced stimulation of pituitary-adrenal activity is mediated by beta adrenoceptors
and involves release of CRF, because it can be prevented by beta-adrenoceptor
blockers and by destruction of CRF neurons (hypothalamic lesions), blockade of
CRF release (chlorpromazine, morphine, and Nembutal), or administration of CRF
antiserum. Although stress can cause a vast increase in plasma E, circulating
E is not essential for the acute stress-induced release of ACTH because blockade
of beta (or alpha) adrenoceptors, administration of chlorisondamine, or extirpation
of the adrenal medulla and sympathectomy do not prevent the pituitary-adrenal
response to stress. In contrast, circulating E plays a major role in the release
of intermediate-lobe peptides during emotional stress. Studies of the role of
AVP in pituitary-adrenal control by the use of pressor receptor (V1) antagonists
are not valuable because of the ineffectiveness of such antagonists in blocking
AVP-induced release of ACTH from corticotropic cells in vitro. Treatment of rats
with an antiserum to AVP reduces the ACTH response to stress. We conclude that
AVP has an important role in stress-induced activation of the pituitary-adrenal
system, possibly by potentiating the effects of CRF." [Abstract] Ordway
GA, Gambarana C, Frazer A.
Quantitative autoradiography of central
beta adrenoceptor subtypes: comparison of the effects of chronic treatment with
desipramine or centrally administered l-isoproterenol.
J Pharmacol Exp Ther 1988 Oct;247(1):379-89
"This study compares the
regulation of the subtypes of central beta adrenoceptors produced by treatment
of rats with desipramine (10 mg/kg i.p. twice daily for 10 days) to that caused
by central infusion of l-isoproterenol (5 micrograms/hr for 7 days). Beta adrenoceptors
were measured by quantitative autoradiography of the binding of [125I]iodopindolol
([125I]IPIN) to coronal sections of rat brain as well as the binding of this radioligand
to homogenates of certain areas of brain. Administration of desipramine caused
significant reductions in the total specific binding of [125I]IPIN in many areas
of the brain, including regions of the amygdala, cerebral cortex, hippocampus,
hypothalamus and thalamus." [Abstract]
Ko
HC, Lu RB, Shiah IS, Hwang CC.
Plasma free 3-methoxy-4-hydroxyphenylglycol
predicts response to fluoxetine.
Biol Psychiatry 1997 Apr
1;41(7):774-81
"This study was designed to investigate the relationship
between platelet serotonin (5-HT) and plasma free 3-methoxy-4-hydroxyphenylglycol
(MHPG) measures in depressed outpatients obtained from the same patient with unipolar
depression during the pretreatment period and subsequent response to 6 weeks of
treatment with either fluoxetine or maprotiline. Compared to the nonresponder
group, the fluoxetine responders showed significantly higher pretreatment levels
of MHPG, but no difference in pretreatment 5-HT levels. There were no significant
differences in either 5-HT or MHPG levels between maprotiline responders and nonresponders.
As to posttreatment levels, there were no between-group differences in 5-HT or
MHPG between responders and nonresponders to either fluoxetine or maprotiline.
When the relationships between changes in 5-HT or MHPG levels and treatment response
were examined, 5-HT values showed a marked decrease in both fluoxetine responders
and nonresponders, but no significant changes were found in the maprotiline treatment
groups. On the other hand, MHPG levels in the fluoxetine nonresponders tended
to increase (borderline significance), whereas the MHPG levels for fluoxetine
responders and maprotiline responders and nonresponders were unaffected from pre-
to posttreatment. Pretreatment levels of plasma free MHPG appear to predict response
to fluoxetine." [Abstract] De
Bellis MD, Geracioti TD Jr, Altemus M, Kling MA.
Cerebrospinal fluid
monoamine metabolites in fluoxetine-treated patients with major depression and
in healthy volunteers.
Biol Psychiatry 1993 Apr 15-May
1;33(8-9):636-41
"Cerebrospinal fluid (CSF) levels of the monoamine metabolites
5-hydroxyindoleacetic acid (5-HIAA), 3-methoxy-4-hydroxyphenylglycol (MHPG), and
homovanillic acid (HVA) were measured in three groups: 46 healthy volunteers;
9 medication-free patients with DSM III-R major depressive disorder, recurrent;
and these same 9 patients following at least 4 weeks of fluoxetine treatment at
20 mg/day. CSF monoamine metabolite levels in medication-free patients did not
differ from healthy volunteers; however, CSF 5-HIAA and MHPG decreased significantly
from 95.9 +/- 24.6 (all values +/- SD) to 64.2 +/- 26.1 pmol/ml and from 46.7
+/- 14.2 to 42.6 +/- 11.6 pmol/ml, respectively, following fluoxetine treatment.
Fluoxetine also significantly decreased mean Hamilton Depression Rating Scale
scores from 23.2 +/- 6.5 to 17.4 +/- 5.0 and significantly increased the CSF HVA/5-HIAA
ratio." [Abstract]
Sheline Y, Bardgett ME, Csernansky JG.
Correlated
reductions in cerebrospinal fluid 5-HIAA and MHPG concentrations after treatment
with selective serotonin reuptake inhibitors.
J Clin Psychopharmacol
1997 Feb;17(1):11-4
"We sought to determine whether fluvoxamine and fluoxetine,
two different antidepressants with in vitro selectivity for the serotonin uptake
transporter also demonstrated similar selectivity in vivo. To accomplish this,
we measured cerebrospinal fluid (CSF) concentrations of 5-hydroxyindoleacetic
acid (5-HIAA), 3-methoxy-4-hydroxyphenylglycol (MHPG), and homovanillic acid (HVA)
before and after 6 weeks of treatment with these two drugs. Twenty-four subjects
who had major depression according to DSM-III-R criteria gave written, informed
consent for the collection of CSF during a double-blind comparative treatment
trial of fluvoxamine (50-150 mg/day) and fluoxetine (20-80 mg/day). The symptoms
of subjects were assessed clinically on a weekly basis throughout the treatment
trial. CSF samples were obtained after a 7- to 14-day washout period before treatment
and again at the end of treatment. CSF samples were analyzed for 5-HIAA, HVA,
and MHPG using high-pressure liquid chromatography coupled to electrochemical
detection. Fluvoxamine- and fluoxetine-treated patients did not differ in clinical
outcome or in the CSF concentrations of monoamine metabolite levels before or
after treatment. Therefore, the CSF data were pooled. Drug treatment, overall,
was associated with significant decreases in 5-HIAA and MHPG and a trend toward
a reduction in HVA levels. Levels of 5-HIAA, MHPG, and HVA were reduced by 57%,
48%, and 17%, respectively. In addition, the magnitude of the decreases in 5-HIAA
and MHPG appeared to be correlated (r = 0.83) across the subjects, although a
Spearman rank correlation indicated that outlying values had an undue effect on
this relationship. These results suggest that treatment with selective serotonin
reuptake inhibitors, which are selective for serotonin uptake in vitro, does not
show a similarly selective effect on serotonin in vivo during treatment of patients."
[Abstract] Widerlov
E, Bissette G, Nemeroff CB.
Monoamine metabolites, corticotropin
releasing factor and somatostatin as CSF markers in depressed patients.
J Affect Disord 1988 Mar-Apr;14(2):99-107
"CSF samples from ten healthy
volunteers and 22 patients with major depression were collected by lumbar puncture
at 9 a.m. and the content of monoamine metabolites, corticotropin releasing factor
(CRF) and somatostatin (SRIF) was analyzed. Plasma concentrations of TSH following
a TRH challenge test (200 micrograms) and plasma cortisol following dexamethasone
(1 mg; DST) were also analyzed. No relationships were observed between the CRF
or SRIF concentrations and either basal or post-dexamethasone cortisol concentrations.
Fourteen of 21 depressed patients were DST nonsuppressors using a plasma cortisol
concentration cut off point greater than or equal to 138 nmol/l. If a more conservative
cut off point was used (greater than 290 nmol/l) seven out of 21 patients revealed
a severity-related cortisol nonsuppression. No significant difference was observed
between healthy volunteers and depressed patients with regard to TSH response
to TRH. The CSF content of CRF was elevated and the content of SRIF reduced in
the depressed patients. In the healthy volunteers an inverse relationship was
observed between CSF concentrations of CRF and MHPG (r = -0.72; P = 0.019); no
relationship was observed between the concentrations of CRF and 5-HIAA or HVA.
In the depressed patients positive correlations were found between CSF concentrations
of CRF and 5-HIAA (r = 0.59; P = 0.004) and between CRF and HVA (r = 0.44; P =
0.042). These data are concordant with the view that norepinephrine and serotonin
may be involved in the regulation of CRF secretion." [Abstract] Jorgensen
H, Knigge U, Kjaer A, Moller M, Warberg J.
Serotonergic Stimulation
of Corticotropin-Releasing Hormone and Pro-Opiomelanocortin Gene Expression.
J
Neuroendocrinol 2002 Oct;14(10):788-795
"The neurotransmitter serotonin
(5-HT) stimulates adrenocorticotropic hormone (ACTH) secretion from the anterior
pituitary gland via activation of central 5-HT1 and 5-HT2 receptors. The effect
of 5-HT is predominantly indirect and may be mediated via release of hypothalamic
corticotropin-releasing hormone (CRH). We therefore investigated the possible
involvement of CRH in the serotonergic stimulation of ACTH secretion in male rats.
Increased neuronal 5-HT content induced by systemic administration of the precursor
5-hydroxytryptophan (5-HTP) in combination with the 5-HT reuptake inhibitor fluoxetine
raised CRH mRNA expression in the paraventricular nucleus (PVN) by 64%, increased
pro-opiomelanocortin (POMC) mRNA in the anterior pituitary lobe by 17% and stimulated
ACTH secretion five-fold. Central administration of 5-HT agonists specific to
5-HT1A, 5-HT1B, 5-HT2A or 5-HT2C receptors increased CRH mRNA in the PVN by 15-50%,
POMC mRNA in the anterior pituitary by 15-27% and ACTH secretion three- to five-fold,
whereas a specific 5-HT3 agonist had no effect. Systemic administration of a specific
anti-CRH antiserum inhibited the ACTH response to 5-HTP and fluoxetine and prevented
the 5-HTP and fluoxetine-induced POMC mRNA response in the anterior pituitary
lobe. Central or systemic infusion of 5-HT increased ACTH secretion seven- and
eight-fold, respectively. Systemic pretreatment with the anti-CRH antiserum reduced
the ACTH responses to 5-HT by 80% and 64%, respectively. It is concluded that
5-HT via activation of 5-HT1A, 5-HT2A, 5-HT2C and possibly also 5-HT1B receptors
increases the synthesis of CRH in the PVN and POMC in the anterior pituitary lobe,
which results in increased ACTH secretion. Furthermore, the results indicate that
CRH is an important mediator of the ACTH response to 5-HT." [Abstract]
Contesse V, Lefebvre H, Lenglet S, Kuhn JM, Delarue
C, Vaudry H.
Role of 5-HT in the regulation of the brain-pituitary-adrenal
axis: effects of 5-HT on adrenocortical cells.
Can J Physiol
Pharmacol. 2000 Dec;78(12):967-83. [Abstract] Fuller
RW.
Serotonin receptors and neuroendocrine responses.
Neuropsychopharmacology
1990 Oct-Dec;3(5-6):495-502
"There is extensive pharmacologic evidence
that serotonin receptors in the brain can activate the hypothalamic-pituitary-adrenocortical
(HPA) axis in rats. Direct-acting serotonin agonists, serotonin uptake inhibitors,
serotonin releasers and the serotonin precursor L-5-hydroxytryptophan all increase
adrenocorticotrophin (ACTH) and corticosterone release. Serotonin-containing nerve
terminals make synaptic contact with corticotrophin-releasing factor (CRF)-containing
cells in rat hypothalamus, and serotonin and serotonin agonists stimulate CRF
release from isolated rat hypothalamus in vitro. Current evidence, based partly
on the ability of selective serotonin receptor antagonists to prevent the increases
in ACTH and corticosterone in rats in vivo, implicates 5-HT1A and 5-HT2/5-HT1C
receptor subtypes in regulating CRF secretion." [Abstract]
[Serotonin 5-HT1C receptors are now referred to as 5-HT2C receptors.] Damjanoska
KJ, Van de Kar LD, Kindel GH, Zhang Y, D'Souza DN, Garcia F, Battaglia G, Muma
NA.
Chronic fluoxetine differentially affects 5-hydroxytryptamine
(2A) receptor signaling in frontal cortex, oxytocin- and corticotropin-releasing
factor-containing neurons in rat paraventricular nucleus.
J
Pharmacol Exp Ther. 2003 Aug;306(2):563-71. Epub 2003 Apr 29.
"Differential
adaptive changes in serotonin2A [5-hydroxytryptamine (5-HT)2A] receptor signaling
during treatment may be one mechanism involved in the latency of therapeutic improvement
with antidepressants, such as fluoxetine. We examined the effects of fluoxetine
(2, 3, 7, 21, or 42 days) on hypothalamic 5-HT2A receptor signaling. The hormone
responses to an injection of the 5-HT2A receptor agonist (+/-)-1-(2,5-dimethoxy-4-iodophenyl)-2-amino-propane
HCl (DOI) were used as an index of hypothalamic 5-HT2A receptor function. Treatment
with fluoxetine for 21 or 42 days produced diminished adrenocorticotropic hormone
(ACTH) and oxytocin (but not corticosterone) responses to DOI injections (2.5
mg/kg i.p.; 15 min postinjection). Regulators of G protein signaling 4 and Galphaq
protein levels in the hypothalamic paraventricular nucleus were not altered during
fluoxetine treatment. Because previous studies indicate that treatment with fluoxetine
for 21 days resulted in increased hormone responses to DOI when measured at 30
min after injection, we examined the effect of fluoxetine (21 days) on DOI-induced
increase hormone levels at 15, 30, and 60 min after DOI injection. Fluoxetine
decreased the oxytocin response at 15 but not at 30 min post-DOI injection, and
potentiated the ACTH and corticosterone responses at 30 min post-DOI injection.
For comparison, we examined the effect of fluoxetine on 5-HT2A receptor-mediated
increase in phospholipase C (PLC) activity in the frontal cortex. 5-HT-stimulated,
but not guanosine 5'-O-(3-thio)triphosphate-stimulated PLC activity was increased
after 21 days of fluoxetine-treatment. Overall, these results indicate that chronic
fluoxetine treatment can potentiate 5-HT2A receptor signaling in frontal cortex
but differentially alters 5-HT2A receptor signaling in oxytocin-containing neurons
and corticotropin-releasing factor-containing neurons in the paraventricular nucleus."
[Abstract]
Owens
MJ, Knight DL, Ritchie JC, Nemeroff CB.
The 5-hydroxytryptamine2
agonist, (+-)-1-(2,5-dimethoxy-4-bromophenyl)-2-aminopropane stimulates the hypothalamic-pituitary-adrenal
(HPA) axis. II. Biochemical and physiological evidence for the development of
tolerance after chronic administration.
J Pharmacol Exp
Ther 1991 Feb;256(2):795-800
"In order to investigate the long term effects
of the 5-hydroxytryptamine2 (5-HT2) receptor agonist, (+-)-1-(2,5-dimethoxy-4-bromophenyl)-2-aminopropane
(DOB), on hypothalamic-pituitary-adrenal (HPA) axis activity, DOB (0.35 mg/kg/day)
was administered via osmotic minipumps to rats for 7 days at which time plasma
adrenocorticotrophic hormone (ACTH), corticosterone and regional brain corticotropin-releasing
factor (CRF) concentrations were measured. In addition, anterior pituitary CRF
and frontal cortical 5-HT2 receptor binding was measured. Seven-day infusion of
DOB resulted in tolerance to the stimulatory actions of the drug on the HPA axis
as evidenced by the return of plasma ACTH and corticosterone concentrations to
base-line values. Moreover, rats treated chronically with DOB exhibited decreased
numbers of both anterior pituitary CRF and cortical and hypothalamic 5-HT2 receptor.
These receptor changes were physiologically significant as challenges doses of
DOB or CRF resulted in blunted ACTH responses. Chronic DOB infusion was without
effect on CRF concentrations in all hypothalamic and extrahypothalamic brain regions
studied. A series of time course experiments revealed that DOB-induced increases
in plasma corticosterone returned to base-line by 2-days postimplantation. This
effect was apparently associated with down-regulation of the 5-HT2 receptor because
high-affinity cortical [3H]DOB and hypothalamic (+-)-[125I]-1-(2,5-dimethoxy-4-iodophenyl)-2-amino-propane
binding were decreased at this time as well. Although median eminence CRF content
was unchanged at all time points, anterior pituitary CRF receptor binding was
significantly decreased 7 days postimplantation." [Abstract] Moncek
F, Duncko R, Jezova D.
Repeated citalopram treatment but not stress
exposure attenuates hypothalamic-pituitary-adrenocortical axis response to acute
citalopram injection.
Life Sci. 2003 Feb 7;72(12):1353-65.
"Many
experimental, clinical and epidemiological studies have shown a direct connection
between exposure to stress or adverse life events and disease, but little is known
about the effect of stress on the action of drugs. The aim of this study was to
test the hypothesis that previous exposure to stress changes the action of the
antidepressant drug citalopram (10 mg/kg, i.p.) on hypothalamic-pituitary-adrenocortical
(HPA) axis function, gene expression of selected neuropeptides and serotonin reuptake.
Three different stress models were used, which included immobilization, restraint
and unpredictable stress stimuli. Samples of plasma for hormone measurement were
taken from conscious cannulated animals. Changes in corticotropin-releasing hormone
(CRH) and proopiomelanocortin (POMC) gene expression in the paraventricular nucleus
of the hypothalamus and the anterior pituitary, respectively, and the ability
of citalopram to inhibit serotonin reuptake were investigated. The exposure to
three different stress models did not influence citalopram action on individual
parameters of HPA axis and on serotonin reuptake. On the other hand, repeated
administration of the drug led to significant attenuation of ACTH and CRH mRNA
responses. The present results allow to suggest that the stressors used did not
influence serotonergic neurotransmission to the extent that would modify HPA axis
response to citalopram challenge. Activation of HPA axis by acute citalopram treatment
was found to be accompanied by increased CRH gene expression in the hypothalamus.
Repeated administration of the drug led to the development of tolerance to activation
of central and peripheral components of HPA axis, but not to serotonin reuptake
inhibition." [Abstract]
Neuger
J, Wistedt B, Sinner B, Aberg-Wistedt A, Stain-Malmgren R.
The effect
of citalopram treatment on platelet serotonin function in panic disorders.
Int Clin Psychopharmacol 2000 Mar;15(2):83-91
"We investigated the effect
of the selective serotonin reuptake inhibitor (SSRI) citalopram after 6-8 weeks
and 6 months of treatment on clinical and peripheral indexes for central serotonergic
function: platelet [14C]serotonin uptake and [3H]paroxetine- and [3H]LSD-binding
to platelets membranes in 33 patients with panic disorder. Basal data from patients
were compared with data from a control material consisting of 33 healthy volunteers.
Bmax for platelet [3H]paroxetine binding was significantly lower in patients than
in controls. There were no differences in serotonin uptake or [3H]LSD-binding
between patients and controls. The degree of anxiety and depression was assessed
using the Beck Anxiety Inventory (BAI) and Beck Depression Inventory self-assessment
scales, and the Clinical Anxiety Scale and the Montgomery Asberg Depression Rating
Scale for clinical evaluation. Complete remission was found in one third of the
patients after 6-8 weeks and in two-thirds after 6 months of treatment. The reduction
in assessment scores was parallelled with similar reductions in platelet 5-HT2-receptor
density, [3H]LSD affinity variable (Kd) and Vmax for platelet [14C]5-HT uptake."
[Abstract]
Peroutka, SJ, Snyder, SH
Regulation of serotonin2
(5-HT2) receptors labeled with [3H]spiroperidol by chronic treatment with the
antidepressant amitriptyline
J Pharmacol Exp Ther 1980
215: 582-587
"The properties of 5-HT2 receptor reduction after chronic
antidepressant treatment indicate that this alteration could be associated with
therapeutic response." [Abstract] Sibille,
Etienne, Sarnyai, Zoltan, Benjamin, Daniel, Gal, Judit, Baker, Harriet, Toth,
Miklos
Antisense Inhibition of 5-Hydroxytryptamine2a Receptor Induces
an Antidepressant-Like Effect in Mice
Mol Pharmacol 1997
52: 1056-1063
"The antidepressant-like effect induced by AS oligonucleotide
injection in mice is consistent with the beneficial effect of pharmacological
blockade of the 5-HT2A receptor in dysthymic disorders." [Full
Text] Flugge G.
Effects of cortisol
on brain alpha2-adrenoceptors: potential role in stress.
Neurosci Biobehav Rev 1999 Nov;23(7):949-56
"It has been proposed that
behavioural changes induced by chronic psychosocial stress in male tree shrews
might be related to alterations in the central nervous alpha2-adrenoceptor system.
In the noradrenergic centres of the brain, alpha2-adrenoceptors function as autoreceptors
regulating noradrenaline release. Chronic stress downregulates these receptors
in several brain regions. Since during stress, the activity of the hypothalamus-pituitary-adrenal
axis is increased leading to high concentrations of plasma glucocorticoids, we
investigated whether the effects of chronic stress can be mimicked by cortisol
treatments. Two experiments were performed: a short-term treatment (males were
injected i.v. with 1.5 mg cortisol and brains were dissected 2 h later) and a
long-term treatment (animals received the hormone in their drinking water for
5 days; daily uptake 3-7 mg). The short-term treatment (injection), similar to
the stress effects, downregulated alpha2-adrenoceptors in several brain regions.
In contrast, the long-term oral treatment induced regional receptor upregulation.
These data show: (i) that glucocorticoids regulate alpha2-adrenoceptors in the
brain; (ii) that the duration and/or the route of cortisol application determines
the results: and (iii) that chronic stress effects are not only due to the long-term
glucocorticoid exposure, but also to other elements of the stress response."
[Abstract] Ordway
GA, Schenk J, Stockmeier CA, May W, Klimek V.
Elevated agonist binding
to alpha2-adrenoceptors in the locus coeruleus in major depression.
Biol
Psychiatry. 2003 Feb 15;53(4):315-23.
"BACKGROUND: Recent postmortem studies
demonstrate disrupted neurochemistry of the noradrenergic locus coeruleus (LC)
in major depression (MD). Increased levels of tyrosine hydroxylase and decreased
levels of norepinephrine transporter implicate a norepinephrine deficiency in
the LC in MD. Here we describe a study of alpha2-adrenoceptors in the LC and raphe
nuclei of subjects with MD compared with psychiatrically normal control subjects.
METHODS: The specific binding of p-[125I]iodoclonidine to alpha2-adrenoceptors
was measured at multiple levels along the rostrocaudal extent of the LC in postmortem
tissue from 14 control and 14 MD subjects. In addition, p-[125I]iodoclonidine
binding was measured in the dorsal and median raphe nuclei in the same tissue
sections. RESULTS: The specific binding of p-[125I]iodoclonidine to alpha2-adrenoceptors
was significantly elevated throughout the LC from MD compared with matched control
subjects. No significant differences were observed in p-[125I]iodoclonidine binding
to alpha2-adrenoceptors in the raphe nuclei comparing MD and control subjects.
CONCLUSIONS: Given that alpha2-adrenoceptors are upregulated in laboratory animals
by treatment with drugs that deplete norepinephrine, our findings implicate a
premortem deficiency of brain norepinephrine in the region of the locus coeruleus
in subjects with MD." [Abstract] Gurguis
GN, Vo SP, Griffith JM, Rush AJ.
Platelet alpha2A-adrenoceptor function
in major depression: Gi coupling, effects of imipramine and relationship to treatment
outcome.
Psychiatry Res. 1999 Dec 20;89(2):73-95.
"Studies
suggest alpha2A-adrenoceptors (alpha(2A)AR) dysregulation in major depressive
disorder (MDD). Platelet alpha(2A)ARs exist in high- and low-conformational states
that are regulated by Gi protein. Although alpha(2A)AR coupling to Gi protein
plays an important role in signal transduction and is modulated by antidepressants,
it has not been previously investigated. Alpha2AR density in the high- and low-conformational
states, agonist affinity and coupling efficiency were investigated in 27 healthy
control subjects, 23 drug-free MDD patients and 16 patients after imipramine treatment
using [3H]yohimbine saturation and norepinephrine displacement of [3H]yohimbine
binding experiments. Coupling measures were derived from NE-displacement experiments.
Patients had significantly higher alpha(2A)AR density, particularly in the high-conformational
state, than control subjects. Coupling indices were normal in patients. High pre-treatment
agonist affinity to the receptor in the high-conformational state and normal coupling
predicted positive treatment outcome. Decreased coupling to Gi predicted a negative
treatment outcome. Imipramine induced uncoupling (-11%) and redistribution of
receptor density in treatment responders only, but had no effect on alpha(2A)AR
coupling or density in treatment non-responders. Increased alpha(2A)AR density
may represent a trait marker in MDD. The results provide indirect evidence for
abnormal protein kinase A (PKA) and protein kinase C (PKC) in MDD which may be
pursued in future investigations." [Abstract] Takeda
T, Harada T, Otsuki S.
Platelet 3H-clonidine and 3H-imipramine binding
and plasma cortisol level in depression.
Biol Psychiatry
1989 May;26(1):52-60
"Platelet 3H-clonidine (alpha 2-adrenergic agonist)
binding and 3H-imipramine binding were measured and the Dexamethasone Suppression
Test performed in 17 normal controls and 14 unmedicated depressed patients in
order to clarify the relationship among these three biological markers. Increases
in the Bmax and the Kd for 3H-clonidine binding and decreases in the Bmax for
3H-imipramine binding of the platelets from depressed patients were observed when
compared with controls. There was a significant positive correlation among 3H-clonidine
Bmax, the basal (predexamethasone) plasma cortisol levels, and the severity of
depression, as indicated by the Hamilton Depression Rating Scale. On the other
hand, no significant correlation was observed in 3H-imipramine binding between
the Bmax and the severity of depression or between the Bmax and the basal plasma
cortisol levels. There was no statistically significant correlation between the
Bmax of 3H-clonidine binding and that of 3H-imipramine binding in depression,
but there was a trend toward correlation in normal controls." [Abstract] Gonzalez-Maeso
J, Rodriguez-Puertas R, Meana JJ, Garcia-Sevilla JA, Guimon J.
Neurotransmitter
receptor-mediated activation of G-proteins in brains of suicide victims with mood
disorders: selective supersensitivity of alpha(2A)-adrenoceptors.
Mol
Psychiatry. 2002;7(7):755-67.
"Abnormalities in the density of neuroreceptors
that regulate norepinephrine and serotonin release have been repeatedly reported
in brains of suicide victims with mood disorders. Recently, the modulation of
the [(35)S]GTPgammaS binding to G-proteins has been introduced as a suitable measure
of receptor activity in postmortem human brain. The present study sought to evaluate
the function of several G-protein coupled receptors in postmortem brain of suicide
victims with mood disorders. Concentration-response curves of the [(35)S]GTPgammaS
binding stimulation by selective agonists of alpha(2)-adrenoceptors, 5-HT(1A)
serotonin, mu-opioid, GABA(B), and cholinergic muscarinic receptors were performed
in frontal cortical membranes from 28 suicide victims with major depression or
bipolar disorder and 28 subjects who were matched for gender, age and postmortem
delay. The receptor-independent [(35)S]GTPgammaS binding stimulation by mastoparan
and the G-protein density were also examined. The alpha(2A)-adrenoceptor-mediated
stimulation of [(35)S]GTPgammaS binding with the agonist UK14304 displayed a 4.6-fold
greater sensitivity in suicide victims than in controls, without changes in the
maximal stimulation. No significant differences were found in parameters of 5-HT(1A)
serotonin receptor and other receptor-mediated [(35)S]GTPgammaS binding stimulations.
The receptor-independent activation of G-proteins was similar in both groups.
Immunoreactive densities of G(alphai1/2)-, G(alphai3)-, G(alphao)-, and G(alphas)-proteins
did not differ between suicide victims and controls. In conclusion, alpha(2A)-adrenoceptor
sensitivity is increased in the frontal cortex of suicide victims with mood disorders.
This receptor supersensitivity is not related to an increased amount or enhanced
intrinsic activity of G-proteins. The new finding provides functional support
to the involvement of alpha(2)-adrenoceptors in the pathogenesis of mood disorders."
[Abstract] Siever
LJ, Uhde TW.
New studies and perspectives on the noradrenergic
receptor system in depression: effects of the alpha 2-adrenergic agonist clonidine.
Biol Psychiatry 1984 Feb;19(2):131-56
"In an attempt to understand the
dynamics of noradrenergic function in depression, we evaluated neuroendocrine,
biochemical, cardiovascular, and behavioral responses to the acute intravenous
administration of the alpha 2-adrenergic agonist, clonidine, in depressed patients
and normal controls. Significantly more variance was observed in the depressed
patients than the controls for most indices of basal noradrenergic output including
plasma norepinephrine (NE) and 3-methoxy-4-hydroxyphenylglycol (MHPG). Growth
hormone, plasma MHPG, and heart rate responses to clonidine were reduced in the
depressed patients compared to the controls, all suggesting reduced responsiveness
of alpha 2-adrenergic receptors in depression. Baseline levels of cortisol were
elevated in the depressed patients compared to the controls. Clonidine decreased
cortisol to normal levels in the depressed patients but had little effect in the
controls. Thus the depressed patients manifested a significantly increased cortisol
response to clonidine. These data raise the possibility that the hypercortisolemia
of depression may be related to noradrenergic dysfunction. Clonidine also significantly
reduced anxiety in the depressed patients, particularly those with elevated basal
plasma MHPG, but not in controls. These results suggest that diminished alpha
2-adrenergic responsiveness as documented by decreased endocrine, biochemical,
and physiological responses to clonidine may be related to the depressive and
anxiety symptoms as well as the neuroendocrine disturbances characteristic of
many depressed patients." [Abstract] Mokrani
MC, Duval F, Crocq MA, Bailey P, Macher JP.
HPA axis dysfunction
in depression: correlation with monoamine system abnormalities.
Psychoneuroendocrinology 1997;22 Suppl 1:S63-8
"Abnormality of the hypothalamic-pituitary-adrenal
(HPA) axis has been one of the most consistently demonstrated biological markers
of depressive disorder. It has also been proposed that abnormality of monoamine
function plays a role in the pathogenesis of the disorder. In order to examine
the interrelationships of the HPA axis with the dopaminergic, noradrenergic, and
serotoninergic systems, we studied, in 52 medication-free inpatients with DSM-IV
nonpsychotic major depressive disorder, the relationship between dexamethasone
suppression test (DST) status and a series of multihormonal responses to apomorphine
(APO), clonidine (CLO), and D-fenfluramine (FEN) tests. DST nonsuppressors did
not present any difference compared with suppressors in growth hormone (GH) and
cortisol stimulation by APO suggesting that a chronic elevation of cortisol did
not lead to an alteration of dopaminergic activity in this population of nonpsychotic
depressed inpatients. Cortisol and prolactin responses to FEN were comparable
in nonsuppressors and in suppressors. In contrast, GH response to CLO was lower
in DST nonsuppressors than in suppressors (p < .03), suggesting that the HPA
abnormality indicated by a positive DST may be related to alpha 2-adrenoreceptor
dysfunction." [Abstract] Price
LH, Charney DS, Rubin AL, Heninger GR.
Alpha 2-adrenergic receptor
function in depression. The cortisol response to yohimbine.
Arch Gen Psychiatry 1986 Sep;43(9):849-58
"There is evidence that the
abnormalities in hypothalamic-pituitary-adrenal (HPA) axis function observed in
patients with depression may be related to changes in central neurotransmitter
receptor function. To evaluate this possibility further, the alpha 2-adrenergic
receptor antagonist yohimbine hydrochloride, which increases brain norepinephrine
turnover, was administered to 40 patients with DSM-III major depression (18 melancholic,
22 nonmelancholic) and 16 healthy controls. Plasma free 3-methoxy-4-hydroxyphenylglycol
(MHPG) level was measured as an index of noradrenergic function, and plasma cortisol
level was used to assess the HPA response. Baseline cortisol levels were elevated
in melancholic depressed patients, but not in nonmelancholic patients, when compared
with healthy controls. The cortisol response to yohimbine was significantly greater
in depressed patients than in controls, despite similar MHPG responses between
groups. Since there is evidence that stimulation of postsynaptic alpha 2-adrenergic
receptors inhibits HPA axis function, the abnormally increased cortisol response
to the alpha 2-antagonist yohimbine suggests a relative subsensitivity of postsynaptic
alpha 2-adrenergic receptors in depression." [Abstract] |