Bipolar Disorder Clinical Trial
Official title:
An Investigation of the Efficacy of the Glutamate Transporter GLT 1 in the Treatment of Bipolar Depression
This study examines if Ceftriaxone, an antibiotic, will improve symptoms of depression in
Bipolar Disorder.
Purpose: This study will examine whether the drug ceftriaxone can help patients with bipolar
depression during short-term treatment of symptoms such as depressed mood, psychomotor
retardation (slowed down thinking and movements), and problems with sleep. Recent studies
suggest that abnormalities in the brain levels of the chemical glutamate may be involved in
causing depression. Ceftriaxone increases a protein in the brain called GLT1, which is
responsible for regulating brain levels of glutamate.
People between 18 and 65 years of age with bipolar disorder who are currently in a depressive
episode of at least 4 weeks but no longer than 12 months duration may be eligible for this
study.
Participants are admitted to the NIH Clinical Center for about 10 weeks. During the first 1
to 2 weeks, they are evaluated and tapered off any antidepressant or mood stabilizers they
have been taking. They remain free of all medication for 2 weeks and are then randomly
assigned to take either ceftriaxone or placebo for 6 weeks. The study drugs are given
intravenously (through a vein) every day. To minimize discomfort, patients are given a PICC
line - a tube that is inserted in a vein in the arm and remains there for the duration of
drug treatment. This prevents the need for repeated intravenous injections.
Patients have a physical examination at the beginning and at the end of the study and two
electrocardiograms (ECG) during the study. They are evaluated periodically with a series of
psychiatric rating scales to determine the effects of the study drug on mood and thinking and
they have periodic blood tests to assess their health status.
In addition, patients are asked to undergo a lumbar puncture (spinal tap) twice during the
study to collect a sample of cerebrospinal fluid (CSF, the fluid that bathes the brain and
spinal cord). The CSF is examined to try to understand how brain chemicals are related to
depression and to the effects of ceftriaxone. A local anesthetic is given and a needle is
inserted in the space between the bones in the lower back where the CSF circulates below the
spinal cord. A small amount of fluid is collected through the needle. This test is optional.
At the end of the study patients are offered free treatment for up to 3 months with standard
medications for bipolar depression and a referral to a community physician for long-term
treatment will be made.
Bipolar affective disorder (BPD, manic-depressive illness) is a common, severe, chronic and
often life-threatening illness. Increasingly, it is being recognized that it is the
depressive phase of the illness, which contributes much of the morbidity and mortality. To
date, only a few of the available somatic treatments have been proven to be effective for the
acute phase of bipolar depression. Thus, there is a clear need to develop novel and improved
therapeutics for bipolar depression. Recent preclinical studies suggest that antidepressants
may exert delayed indirect effects on the glutamatergic system. Clinical data suggests that
glutamatergic modulators may have antidepressant effects in humans. We first tested the
glutamatergic modulator riluzole, an inhibitor of glutamate release and enhancer of glutamate
reuptake in astrocytes and found it to have antidepressant properties in patients with
treatment-resistant major depression and bipolar depression. In a recent study, we found that
a single intravenous dose of the non-competitive NMDA antagonist ketamine produced a rapid
and relatively sustained antidepressant effect in patients with treatment-resistant major
depression. A recent report found that the Beta-lactam antibiotic ceftriaxone increased
uptake of glutamate via increased GLT1 function (Rothstein et al 2005) and had
antidepressant-like effects in animal models (Mineur et al 2006). Together, these data
suggest that the glutamatergic system may play a role in the pathophysiology and treatment of
depression, and that agents which more directly reduce glutamatergic neurotransmission may
represent a novel class of antidepressants.
We propose to expand our previous findings on the efficacy of glutamatergic modulators in
patients with unipolar and bipolar depression by testing a specific, new mechanism where by
we use ceftriaxone to chronically increase the expression of the glutamate transporter GLT1
in order to facilitate the removal of glutamate from the synaptic cleft in an effort to
reduce excessive glutamate transmission and as a result produce acute antidepressant effects.
The model presented here is a clinical testable one, and one that, if successful, holds the
potential to develop a group of novel pharmacological treatments for major depression.
Patients, ages 18 to 65, with a diagnosis of bipolar depression (without psychotic features),
will be randomized to double-blind treatment to receive either ceftriaxone (1-4 g/day) or
placebo intravenously for a period of 6 weeks. Acute efficacy will be determined by
demonstrating a greater response rate using specified criteria. Approximately 86 patients
with bipolar depression will be enrolled in the study.
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