A collaborative study led by investigators from MGH is giving what may be the first look at how interactions between genes underlie a key symptom of schizophrenia, impaired working memory.
Interaction between gene variants may alter brain function in schizophrenia
Imaging study is one of the first to analyze influence of multiple genes
07/Nov/2008
A
collaborative study led by investigators from Massachusetts General Hospital
(MGH) is giving what may be the first look at how interactions between genes
underlie a key symptom of schizophrenia, impaired working memory. Functional imaging studies reveal how a
combination of common variants in two genes is associated with reduced activity
of important brain structures in schizophrenia patients but not in normal controls. The report has been released online in the
Early Edition of the Proceedings of the National Academy of Sciences.
“Schizophrenia
is a highly genetic disorder, but we are learning that its genetics are not
straightforward. In most cases potential
risk genes appear to have very small effects on symptoms, making it difficult
to attribute clinical findings to particular genes,” says Joshua Roffman, MD,
of the MGH Department of Psychiatry, the study’s lead author. “To amplify some of these subtle effects, we
and others are looking how the genes affect brain function, rather than just
behavior.”
The team –
which included investigators from the University of New Mexico, University of
Iowa and University of Minnesota through the MIND Clinical Imaging Consortium –
used functional MRI to scan an area of the prefrontal cortex known to be
critical to working memory in 79 schizophrenia patients and 75 healthy controls
as they completed a memory task. Levels
of cortical activity were then analyzed for any association with common
variants in two genes: MTHFR, which regulates folate metabolism and has been
associated with schizophrenia risk, and COMT, which is involved with dopamine
processing during working memory.
Although
the schizophrenia-associated variant of MTHFR was found in both patients and
controls, when the working memory task become more difficult, weaker cortical
function associated with that variant was seen only in the schizophrenia
patients, not in controls. While variations
in COMT did not influence cortical activation patterns on their own, the
combined effects of both genes did make a difference. The reduction in cortical function seen in
patients with the schizophrenia-associated MTHFR variant was even more
pronounced in patients who also had a COMT variant previously associated with
less efficient working-memory-related brain activity.
“Based on
the known effects of these alleles on brain biochemistry, it is likely that our
results reflect cumulative impacts of the gene variants on dopamine signaling,
particularly in the prefrontal cortex.
These findings may help us to identify patients more likely to benefit
from new treatments targeting the dopamine and folate systems,” Roffman
says. “We are hopeful that this approach
will catalyze the development of individualized treatment regimens, since it
will allow us to examine the effects of treatment-related genes on brain
function using a much smaller groups of study participants.”
Roffman is
an instructor in Psychiatry at
link to MGH
schizophrenia program
Media Contacts: Sue McGreevey, smcgreevey@partners.org, 617 724-2764

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