Bipolar Disorder Clinical Trial
Official title:
Pilot Evaluation of Levetiracetam (Keppra® (Registered Trademark)) in Bipolar Illness
This study will explore the possible effectiveness of levetiracetam in patients with bipolar
illness who have not responded adequately to standard treatments. Levetiracetam was recently
approved to treat seizures. Other drugs in the same class as levetiracetam, including
carbamazepine and valproate, are widely recognized as substitute medications for lithium or
are used as an adjunct to it, and other anticonvulsants have also shown promise in improving
bipolar symptoms.
Patients with bipolar illness whose manic, depressed or unstable moods are not adequately
controlled by their current treatment and who have not responded previously to two standard
treatments (i.e., lithium, valproate, carbamazepine or neuroleptics) may be eligible for
this study.
Participants will take levetiracetam starting at 500 mg daily. If this dose is well
tolerated, it will be increased to 500 mg twice a day. Every 3 days, doses may be increased
until the target dose of 3000 mg/day is reached. Higher doses, not to exceed 4000 mg/day,
may be tried in patients who do not respond fully to the lower doses. Patients and observers
will use standard ratings to evaluate the patients' response to therapy during the 8-week
study. If, after 8 weeks, the results appear promising, patients may continue treatment for
an additional 6 months to evaluate longer-term effects.
Almost all of the approved anticonvulsant compounds (with the exception of gabapentin and
tiagabine) have now been suggested to have acute antimanic or more long-term mood
stabilizing properties. Carbamazepine and valproate have gained a widely recognized role in
treatment algorithms of bipolar illness, and lamotrigine has shown promising antidepressant
effects. Levetiracetam (Keppra® (Registered Trademark)) is the most recently approved
anti-epileptic drug available, and deserves pilot exploration in bipolar illness for a
variety of reasons. These include: its positive side-effects profile; it is a derivative of
the nootropic agent piracetam which has memory-enhancing properties in animal studies; it
likely has a unique mechanism of action since it is not active on most of the traditional
excitatory and inhibitory neurotransmitter systems; it is not active on traditional
anticonvulsant models such as pentylenetetrazol (PTZ) or maximum electroshock (MES)
seizures, but is able to stop both the development and completed phase of amygdala-kindled
seizures; and it is not metabolized by hepatic enzymes and thus has few adverse
pharmacokinetic interactions.
We propose pilot exploration of levetiracetam as an adjunctive agent in patients with
bipolar illness who are inadequately responsive to routine psychopharmacological agents for
bipolar illness. At the NIMH we will study a maximum of 10 acutely depressed, 10 manic, and
10 cycling patients enrolled in Protocol 97-M-0039. We would start at Levetiracetam doses of
500 mg/day, and not to exceed 4000 mg/day. Response will be based primarily on the
percentage of patients showing "much" or "very much" improvement on the GCI-BP score in each
of the three groups as augmented by the percentage decrement on cross-sectional scales such
as the Inventory of Depressive Symptomatology (IDS) and Young Mania Rating Scale (YMRS) in
conjunction with prospective ratings on the NIMH-LCMp. Should preliminary evidence of
efficacy be observed in this open add-on clinical trial, more systematic controlled studies
will then be designed for confirmation of promising target areas of efficacy.
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Endpoint Classification: Safety/Efficacy Study, Primary Purpose: Treatment
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