Bipolar Disorder Clinical Trial
Official title:
A Double-Blind Study Examining the Efficacy of the Protein Kinase C Inhibitor Tamoxifen in the Treatment of Acute Mania
The purpose of this study is to examine how the drug tamoxifen affects the brain in patients
with bipolar I disorder.
Bipolar Disorder (BD) is a severe, chronic, and often life-threatening illness for which safe
and effective treatments are necessary. The mood stabilizing effects of lithium and valproate
have revolutionized the treatment of patients with BD. However, a significant percentage of
patients do not respond fully to these drugs, and the biochemical basis for the antimanic and
mood-stabilizing actions of lithium and valproate is unclear. Both drugs inhibit protein
kinase C (PKC). There is a need to investigate the efficacy of a direct PKC inhibitor in the
treatment of acute mania. Tamoxifen is currently the only relatively selective PKC inhibitor
available for human use.
Participants in this study will be screened with a physical, psychiatric, and eye examination
and blood and urine tests. Eligible participants will be hospitalized at the Clinical Center
for at least 4 weeks. They will be tapered off all psychiatric medication and kept drug free
for 2 to 7 days. They will also be put on a low-monoamine, low-caffeine diet. Participants
will be randomly assigned to receive either tamoxifen or placebo (an inactive pill) for 3
weeks. During this time, participants will have daily pulse and blood pressure measurements,
several electrocardiograms (EKGs), and blood draws. Weight measurements will be taken at
least twice during the study, and caffeine or dextromethorphan will be given at the beginning
and end of the study to test how tamoxifen affects the way the body eliminates other
medications. Participants will have a physical examination at the end of the study.
At the end of this 4-week study, some participants may continue the study and will receive
tamoxifen for an additional 3 weeks. At the conclusion of the study, participants'
psychiatric status will be reassessed and long-term psychiatric treatment for their mood
disorders will be arranged.
Bipolar Disorder (BD) is a common, severe, chronic and often life-threatening illness.
Suicide is the cause of death in 10-20% of individuals with BD. The discovery of lithium's
efficacy as a mood-stabilizing agent has since revolutionized the treatment of patients with
BD. However, approximately 50% of patients do not respond fully to lithium, and the
biochemical basis for lithium's antimanic and mood-stabilizing actions remains to be fully
elucidated. Elucidation of the mechanism(s) by which lithium stabilizes an underlying
dysregulation of limbic and limbic-associated function also offers the potential to delineate
the underlying pathophysiology of BD; however, a major problem inherent in neuropharmacologic
research is the difficulty in attributing therapeutic relevance to any observed biochemical
finding. One powerful approach is to identify common biochemical targets, which are modified
by drugs belonging to the same therapeutic class (e.g. mood-stabilizing agents) but
possessing distinct chemical structures when administered in a therapeutically relevant
paradigm (i.e., effects which are observed upon chronic drug administration, and yet persist
beyond abrupt drug discontinuation). In this context, it is noteworthy that both valproic
acid (VPA) and lithium, with different chemical structures, belong to the same therapeutic
class and cause considerable inhibition of protein kinase C (PKC). The PKC signaling pathway
is clearly a target for the actions of two structurally highly dissimilar antimanic agents --
lithium and VPA. Do these effects of lithium and VPA on PKC signaling have any clinical
relevance? There is thus a clear need to investigate the potential efficacy of a direct PKC
inhibitor in the treatment of acute mania. There is currently only one relatively selective
PKC inhibitor available for human use- Tamoxifen. Tamoxifen (TAM), a synthetic nonsteroidal
antiestrogen, has been widely used in the treatment of breast cancer. TAM's potent inhibitory
effects on PKC are striking. Recently, our group conducted the first open-label study with
TAM in acute mania. In this study, TAM resulted in a significant decrease in manic symptoms
within a short period of time (3-7 days).
The overarching goal of this proposal is to test the hypothesis that PKC inhibition is part
of the mechanism of the therapeutic effect of mood stabilizing drugs. The proposal derives
from and builds on our published open-label study of TAM in acute mania (Bebchuk et al.,
2000). However, the efficacy of TAM monotherapy in acute mania has only been reported in an
open-label study and has not yet been evaluated in a randomized, double blind,
placebo-controlled study.
Male or female patients, ages 18 to 65, with a diagnosis of bipolar I disorder manic or mixed
(with or without psychotic features), will be randomized to double-blind treatment to receive
either TAM (20-140 mg/day) or placebo, for a period of 3 weeks. Following this acute period,
the patients will receive either open-label TAM or treatment as clinically indicated.
Approximately 50 patients with acute mania will be enrolled in the study. Biochemical
measures will be obtained during the study.
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