| City: |
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Bethesda |
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State:
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MD |
| Zip Code: |
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20892 |
| Conditions: |
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Depression - Bipolar Disorder |
| Purpose: |
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The purpose of this study is to use brain imaging technology to examine the role of certain
brain receptors and the nervous system chemical acetylcholine in major depression.
The cholinergic system involves the regulation of neurotransmitters and the brain receptors
to which they bind. Evidence suggests that the cholinergic system may play a role in the
development of depression. Acetylcholine is a neurotransmitter that binds to certain brain
receptors called muscarinic cholinergic receptors. Cholinomimetic drugs (drugs that
stimulate the cholinergic system) often exacerbate depressive symptoms in people with mood
disorders and in healthy individuals. This increase in depressive symptoms may be caused by
stimulation of muscarinic acetylcholine receptors (mAChRs), but further study is needed to
confirm this. This study will use positron emission tomography (PET) and magnetic resonance
imaging (MRI) to study the function of mAChRs in individuals with depression.
Participants in this study will undergo a physical examination, psychiatric interviews,
neuropsychological tests, PET and MRI scans, and rating scales of depression, anxiety, and
negative thinking symptoms. Questions about behavior and functioning will be asked and blood
samples will be collected for genetic analysis.
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| Study summary: |
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Several paths of evidence converge in implicating a role for the cholinergic system in the
pathophysiology of affective illness. In both unipolar depressed and euthymic bipolar
subjects, cholinomimetic drugs (i.e., muscarinic agonists, acetylcholinesterase inhibitors)
exacerbate depressive signs and symptoms such as dysphoria, psychomotor retardation,
impairment of attention and memory, hypothalamic pituitary adrenal axis hyperactivity and
sleep EEG abnormalities. In healthy subjects, the acetylcholinesterase inhibitor
physostigmine elicits a range of depressive symptoms including dysphoria, anergia,
psychomotor slowing, emotional lability, sleep disturbances, memory and concentration
impairment, and with higher doses, tearfulness and depression. These effects have been
shown to reflect stimulation of muscarinic receptors. Cholinomimetics also exacerbate
behavioral despair in putative animal models of depression. Conversely, the anticholinergic
agent biperidine improved symptoms of depression in a placebo controlled study. Moreover,
muscarinic cholinomimetics and a choline rich nutrient, lecithin (phosphatidylcholine) exert
antimanic effects in bipolar subjects.
Potentially consistent with these observations, depressed subjects exhibit hypersensitivity
to cholinomimetic agents. Administration of muscarinic cholinergic agonists, ACh releasing
agents or acetylcholinesterase inhibitors induce exaggerated effects on REM density and
latency in depressed subjects than in healthy controls. In addition, both manic and
depressed bipolar subjects show increased pupillary sensitivity to the muscarinic
cholinergic agonist pilocarpine relative to controls.
Despite the data implicating the mAChR receptor system in mood disorders, no direct in vivo
investigations of the central mAChR have been performed in depressed subjects. A novel PET
radioligand, [(18)F]FP-TZTP was recently developed by Eckelman as a selective agonist of
M(2) receptors. Because the M(2) receptor functions predominately as a presynaptic
release-controlling autoreceptor, decreased distribution volume (V) of this receptor could
conceivably give rise to increased postsynaptic muscarinic receptor sensitivity.
This application proposes a pilot PET study of M(2) receptor distribution volume in
currently depressed subjects with major depressive disorder (n=30), currently depressed
subjects with bipolar disorder (n=30), and psychiatrically healthy controls (n=30). The
proposed pilot study will test the central hypothesis that M(2) receptor V is decreased in
regions where they are primarily located presynaptically in depressed subjects relative to
healthy controls. The proposed study will advance knowledge regarding the pathophysiology
of depression. |
| Criteria: |
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- INCLUSION CRITERIA - MDD Depressed Sample:
Thirty subjects (ages 18-45) male and female will be selected, with primary MDD currently
depressed as defined by DSM-IV criteria for recurrent MDD and current HDRS score in the
moderately-to-severely depressed range (greater than 18) and who have a first degree
relative with MDD but no first degree relatives with mania, alcoholism, or antisocial
personality disorder.
INCLUSION CRITERIA - Bipolar Depressed Sample:
Thirty subjects (ages 18-45) male and female will be selected who meet DSM-IV criteria for
bipolar I or II disorder and are currently depressed, with HDRS score in the
moderately-to-severely depressed range (greater than 18). Subjects may be inpatients or
outpatients. Because effective treatment will not be discontinued for the purposes of
this protocol, subjects will be identified who have never been treated or who have
discontinued medication due to lack of efficacy, noncompliance, physician order, or other
reasons prior to study entry.
INCLUSION CRITERIA - Healthy, Control Sample:
Thirty subjects (ages 18-45) male and female who have not met criteria for any major
psychiatric disorder will be selected. From this large sample a control subject will be
matched to each depressed subject for age, gender, handedness and stage of menstrual
cycle. The control subjects will have no known first degree relatives with mood
disorders.
EXCLUSION CRITERIA:
Subjects must not have taken antidepressant or other medications likely to alter monoamine
neurochemistry or cerebrovascular function for at least 3 weeks (8 weeks for fluoxetine
and for any drug with known anticholinergic effects) prior to scanning. Because effective
medications will not be discontinued for the purposes of this study, subjects will be
identified who have never been treated or who have discontinued medication due to lack of
efficacy, noncompliance, physician order or other reasons prior to study entry. Subjects
will also be excluded if they: a) serious suidical ideation or behavior - 1) thoughts of
suicide within the past three months which are accompanied by intet to harm oneself,
serious consideration of means or plan to attempt suicide, evidence of arranging for a
suicide attemp (e.g. giving away prized possessions, updating a will) or clear desire to
commit suicide; 2) suicide attempts within the previous one year; or 3) a current plan to
inflict self harm or physical evidence suspicious for having engaged in a suicide attempt.
Subjects will also be excluded if they had any significant comorbid condition in the last
year, c) psychosis to the extent that the ability to provide informed consent is in doubt,
d) history of any major psychiatric disorder (other than the target mood disorder) arising
temporally before the initial mood episode, e) medical or neurological illnesses (i.e.
seizure disorder, a coma in past) likely to affect physiology or anatomy, f) a history of
drug or alcohol abuse within 1 year or a lifetime history of alcohol or drug dependence
(DSM IV criteria), g) are HIV positive or have AIDS, h) current pregnancy (documented by
history and pregnancy testing prior to scanning), i) current breast feeding, j) general
MRI exclusion criteria which include the subject having a pacemaker or significant
claustrophobia and k) if they are smokers. |
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If you are interested in this clinical trial please use the contact information above. If you would like to get additional information about this clinical trial please visit ClinicalTrials.gov.
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| Data Source: |
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ClinicalTrials.gov |
| Date Processed: |
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May 10, 2010 |
Modifications to
this listing: |
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Only selected fields are shown, please use the link
above to view all information about this clinical trial. |
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