Major Depression Clinical Trial
Official title:
An Investigation of the Antidepressant Effects of the Selective NR2B Antagonist MK-0657 in Major Depression
Purpose : This study will determine whether MK-0657, a selective NR2B Antagonist, can
quickly improve symptoms of depressed mood, psychomotor retardation, poor motivation and
reduced enjoyment of things in patients with major depression.
MK-0657 decreases the activity of a brain receptor called NMDA, which the chemical glutamate
binds to, possibly inducing a rapid antidepressant response. People between 18 and 55 years
of age who have major depression of at least 4 weeks' duration and have not been helped by
two antidepressants approved for major depression may be eligible for this study. Women who
are able to have children are excluded. Participants are admitted to the NIH Clinical Center
for two study phases, as follows. Phase I (1 to 2 weeks): Patients are tapered off their
current medications. Phase II (7 weeks): Patients are randomly assigned to take either
MK-0657 or placebo (look-alike capsules with no active ingredient) by mouth for 12 days. At
some point during the second part this phase, patients who had been taking MK-0657 are
switched over to placebo and those who had been taking placebo are switched to MK-0657.
Participants undergo the following procedures during the study:Physical examination twice
(at the beginning and at the end of the study) Electrocardiogram (ECG) four times Blood
tests about six times Rating scales up to 28 times to assess the effects of MK-0657 on mood
and thinking Blood pressure measurements three times a day.
Study examines the effectiveness of a new medication, targeting a system called glutamate,
will improve depression when compared with placebo.
Even though there are many antidepressant drugs for clinical use, clinical trials indicate
that 30% to 40% of patients with major depression fail to respond to first-line
antidepressant treatments despite adequate dosage, duration, and compliance. Furthermore,
these medications may take weeks to months to achieve their full effects and in the
meantime, patients continue to suffer from their symptoms and be at risk of self-harm as
well as harm to their personal and professional lives. Thus, there is a clear need to
develop novel and improved therapeutics for treatment-resistant major depression that have a
rapid onset of action. Recent preclinical studies suggest that antidepressants may exert
delayed indirect effects on the glutamatergic system, specifically on the NMDA receptor
complex. A recent study by our group found that a single intravenous dose of the
non-competitive NMDA antagonist ketamine produced a rapid, robust and relatively sustained
antidepressant effect in patients with treatment-resistant major depression. Together, these
data suggest that the NMDA receptor may play an important role in the mechanism of
antidepressant action. Unfortunately, ketamine's psychotomimetic effects preclude its use as
a chronic antidepressant; these side effects probably are a result of ketamine's effects on
multiple NMDA subunits. Thus, studying selective NMDA subunit antagonists in depression is a
reasonable next step. The NR2B subunit stands as a prime candidate to test in depression.
Preclinical data by our group indicates that the NR2B subunit is involved in the mechanism
of antidepressant action as indicated by changes in phosphorylation of serine residues in
the learned helplessness model of depression and with chronic treatment with imipramine. In
addition, we found that the NR2B antagonist R0 25-6981 has antidepressant-like properties in
the forced swim test. We propose to examine whether the selective NR2B antagonist (MK-0657)
produces rapid antidepressant effects in patients with treatment-resistant major depression
but without causing psychotomimetic effects.
Male and female patients, ages 18 to 55 years, with a diagnosis of major depression (without
psychotic features), will be recruited for this study. This study consists of the
double-blind crossover administration of either the NR2B antagonist MK-0657 (4-8 mg/day) or
placebo.
The specific aim of this study is to assess the efficacy of 12 days of a selective NR2B
antagonist (MK-0657, 4-8 mg/day given orally) compared with placebo in improving overall
depressive symptomatology in patients with treatment-resistant major depression.
Our primary hypothesis is that subjects with treatment-resistant major depression who are
randomized to a selective NR2B antagonist (MK-0657) will have a more rapid and superior
response compared to when they are randomized to placebo. This is a proof of concept and
treatment study.
Approximately, 27 subjects will be randomized; the accrual ceiling for this protocol is 60
subjects.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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