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Ed. Note: The following is a press
release from the National Institute Of Mental Health.
March 15, 2006 --
Whether depressed patients will
respond to an antidepressant depends, in part, on which version of a gene
they inherit, a study led by scientists at the National Institutes of Health
(NIH) has discovered. Having two copies of one version of a gene that codes
for a component of the brain’s mood-regulating system increased the odds of
a favorable response to an antidepressant by up to 18 percent, compared to
having two copies of the other, more common version.
Since the less common version was
over 6 times more prevalent in white than in black patients — and fewer
blacks responded — the researchers suggest that the gene may help to explain
racial differences in the outcome of antidepressant treatment. The findings
also add to evidence that the component, a receptor for the chemical
messenger serotonin, plays a pivotal role in the mechanism of antidepressant
action.
The study, authored by National
Institute of Mental Health (NIMH) researchers Francis J. McMahon, M.D.,
Silvia Buervenich, Ph.D., and Husseini Manji, M.D., along with collaborators
at several other institutions, was posted online March 8 and will appear in
the May, 2006 American Journal of Human Genetics.
“This discovery brings us closer
to the day when clinicians will be able to offer treatment options and
medications that are tailored and personalized to be optimally effective for
individual patients,” said NIH Director Elias A. Zerhouni, M.D.
However, the findings cannot yet
guide treatment decisions.
“To our knowledge, this is the
first demonstration of significant, replicated association between genetic
variation and outcome of antidepressant treatment,” added Manji, director of
the NIMH’s Mood and Anxiety Disorders Program.
In the initial phase of the NIMH-funded
STAR*D (Sequenced Treatment Alternatives for Depression) trial, about 47
percent of the 2,876 participants experienced some improvement with the
serotonin selective reuptake inhibitor (SSRI) citalopram (Celexa). The NIH
scientists set out to find genetic factors that might help to explain why
some patients fared better than others.
They screened genetic material
from 1,953 of the STAR*D patients, a sample with a higher percentage of
responders (69 percent), in part because patients who were doing well tended
to stay in contact longer and were more likely to allow a blood sample to be
drawn. The researchers looked for associations between treatment response
and 768 known sites of variability in 68 suspect genes — sites where letters
in the genetic code vary across individuals.
They found the strongest
connection in the gene that codes for the serotonin 2A receptor, one of
several proteins to which serotonin binds when brain cells communicate.
Located on cells in the brain’s
thinking center (cortex), the serotonin 2A receptor regulates circuits
implicated in depression. Antidepressants, including citalopram, reduce the
number of serotonin 2A receptors in animal cortex over the course of a few
weeks — the same time-frame required for the drugs to work in humans —
suggesting that the receptors are important in the drugs’ mechanism of
action.
Everyone inherits two copies of
the serotonin 2A receptor gene, one from each parent. A tiny glitch in the
gene’s chemical sequence results in some people having an adenine (A) at the
same point that other people have a guanine (G). So an individual can have
gene types AA, AG or GG. Overall, the prevalence of the A version was 38
percent, compared to 62 percent for the G version in this sample. Fourteen
percent had AA gene type, 43 percent AG and 43 percent GG. Since the site of
variation is located in a stretch of genetic material with no known
function, the researchers suspect that it may be just a marker for a
still-undiscovered functional variation nearby in the gene.
Based on scores on a depression
rating scale, close to 80 percent of patients who had AA responded to the
antidepressant, compared to about 62 percent of those with GG. Thus,
patients with the AA gene type were 16-18 percent more likely to benefit
from the medication. Even patients with AG showed some increased benefit.
But this only applied to white
patients, in whom the A version was more than six times more frequent than
in black patients. There was no significant association between gene type
and treatment outcome in black patients, who tended to fare less well in the
trial overall.
“We now have to consider genetic
factors as well as psychosocial issues in our attempts to explain why
antidepressants do not help our black patients as much as they should,”
McMahon said. “The new findings help make a compelling case for a key role
of the serotonin 2A receptor in the mechanism of antidepressant action.”
Also participating in the study
were: A. John Rush and Madhukar Trivedi, University of Texas Southwestern
Medical Center; Gonzalo Laje, NIMH; Dennis Charney, Mount Sinai Hospital;
Robert Lipsky, National Institute on Alcohol Abuse and Alcoholism (NIAAA);
Alexander Wilson, Alexa Sorant, and George Papanicolaou, National Human
Genome Research Institute (NHGRI); Maurizio Fava, Massachusetts General
Hospital; and Stephen Wisniewski, University of Pittsburgh.
NIMH, NIAAA and NHGRI are
part of the National Institutes of Health (NIH), the Federal Government's
primary agency for biomedical and behavioral research. NIH and CDC are
components 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
http://www.nih.gov.
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