EXPERIMENTAL MEDICATION KICKS DEPRESSION IN HOURS INSTEAD OF WEEKS

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U.S. Department of Health and Human Services 
NATIONAL INSTITUTES OF HEALTH 
NIH News 
National Institute of Mental Health (NIMH) 
http://www.nimh.nih.gov

EMBARGOED FOR RELEASE: Monday, August 7, 2006; 4:00 p.m. ET 

CONTACT: Susan Cahill, NIMH Press Office (NIMHpress@xxxxxxx),
301-443-4536, 

EXPERIMENTAL MEDICATION KICKS DEPRESSION IN HOURS INSTEAD OF WEEKS 

People with treatment-resistant depression experienced symptom relief in
as little as two hours with a single intravenous dose of ketamine, a
medication usually used in higher doses as an anesthetic in humans and
animals, in a preliminary study. Current antidepressants routinely take
eight weeks or more to exert their effect in treatment-resistant
patients and four to six weeks in more responsive patients -- a major
drawback of these medications. Some participants in this study, who
previously had tried an average of six medications without relief,
continued to show benefits over the next seven days after just a single
dose of the experimental treatment, according to researchers conducting
the study at the National Institutes of Health's National Institute of
Mental Health.

This is among the first studies of humans to examine the effects of
ketamine on depression, a debilitating illness that affects 14.8 million
people in any given year. Used in very low doses, the medication is
important for research, but is unlikely to become a widely used clinical
treatment for depression because of potential side effects, including
hallucinations and euphoria, at higher doses.  However, scientists say
this research could point the way toward development of a new class of
faster- and -longer-acting medications.  None of the patients in this
study, all of whom received a low dose, had serious side effects. Study
results were published in the August issue of the "Archives of General
Psychiatry."

"The public health implications of being able to treat major depression
this quickly would be enormous," said NIH Director Elias A. Zerhouni,
M.D. "These new findings demonstrate the importance of developing new
classes of antidepressants that are not simply variations of existing
medications."

For this study 18 treatment-resistant, depressed patients were randomly
assigned to receive either a single intravenous dose of ketamine or a
placebo (inactive compound). Depression improved within one day in 71
percent of all those who received ketamine, and 29 percent of these
patients became nearly symptom-free within one day. Thirty-five percent
of patients who received ketamine still showed benefits seven days
later. Participants receiving a placebo infusion showed no improvement.
One week later, participants were given the opposite treatment, unless
the beneficial effects of the first treatment were still evident. This
"crossover" study design strengthens the validity of the results. 

"To my knowledge, this is the first report of any medication or other
treatment that results in such a pronounced, rapid, prolonged response
with a single dose. These were very treatment-resistant patients," said
NIMH Director Thomas R. Insel, M.D.

Ketamine blocks a brain protein called the "N"-methyl-D-aspartic acid
(NMDA) receptor.  Previous studies have shown that agents that block the
NMDA receptor reduce depression-like behaviors in animals.

NMDA receptors are critical for receiving the signals of glutamate, a
brain chemical that enhances the electrical flow among brain cells that
is required for normal function. Studies indicate that dysregulation in
glutamate could be among the culprits in depression. Using ketamine to
block glutamate's actions on the NMDA receptor appears to improve
function of another brain receptor -- the AMPA receptor -- that also
helps regulate brain cells' electrical flow.

Scientists think the reason current antidepressant medications take
weeks to work is that they act on targets close to the beginning of a
series of biochemical reactions that regulate mood.  The medications'
effects then have to trickle down through the rest of the reactions,
which takes time.  Scientists theorize that ketamine skips much of this
route because its target, the NMDA receptor, is closer to the end of the
series of reactions in question.

"This may be a key to developing medications that eliminate the weeks or
months patients have to wait for antidepressant treatments to kick in,"
said lead researcher Carlos A. Zarate Jr., of the NIMH Mood and Anxiety
Disorders Program.

The researchers who conducted the study now are zeroing in on other
areas of the glutamate system.  Specifying which components of the
system are affected by compounds such as ketamine may help scientists
understand how and why depression occurs, reveal biological markers that
may one day aid in diagnosis, and point the way to more precise targets
for new medications.

Dr. Zarate was joined in this research by Husseini K. Manji, chief of
the NIMH Mood and Anxiety Disorders Program, and colleagues Jaskaran B.
Singh, Paul J. Carlson, Nancy E. Brutsche, Rezvan Ameli, David A.
Luckenbaugh, and Dennis S. Charney.

NIMH is part of the National Institutes of Health (NIH), the Federal
Government's primary agency for biomedical and behavioral research. NIH
is a component of the U.S. Department of Health and Human Services. 

The National Institutes of Health (NIH) -- "The Nation's Medical
Research Agency" -- includes 27 Institutes and Centers and is a
component of the U.S. Department of Health and Human Services. It is the
primary federal agency for conducting and supporting basic, clinical and
translational medical research, and it investigates the causes,
treatments, and cures for both common and rare diseases. For more
information about NIH and its programs, visit www.nih.gov.
  
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This NIH News Release is available online at:
http://www.nih.gov/news/pr/aug2006/nimh-07b.htm.

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