By Duke Medicine News and Communications
DURHAM, N.C. -- While epilepsy has long been thought to boost
production of new brain cells (neurons)as a means of repairinginjury, a
new study shows that chronic seizures actually decrease new neuron
production in the brain's learning and memory center.
The study
is the first to demonstrate hownew neuron production in the brain's
"hippocampus" is affected by chronic, rather than acute, seizures, said
the researchers from Duke University Medical Center and the Durham VA
Medical Center.The hippocampus is the brain region where learning,
memory and mood are regulated andwhere epilepsy causes injury.
In
the study, ratswith chronic epilepsy showed a 75 percent decrease in
new neuron production in the hippocampus compared to normal animals,
said Ashok K. Shetty, Ph.D., a research professor of neurosurgery at
Duke and the study's senior author.
The finding explains why
chronic epileptics are prone to learning and memory deficits and
depression, hesaid.Epilepsy occurs when electrical signals in the brain
are disrupted, causing uncontrolled body movements and changes in
learning, memory and emotion.
Shetty said their new knowledge of
neuron growth, or neurogenesis, in chronic epilepsy could lead to
treatments thatalleviate the learning and memory deficits and
moodsymptoms that accompany the disease. The findings could potentially
even reduce the prevalence of seizures, he said.
Results of their
study onneurogenesis in rats with epileptic seizures are published in
the December issue of Neurobiology of Disease. Bharathi Hattiangady,
Ph.D., research associate in neurosurgery, is the lead author,and
research associate Muddanna Rao, Ph.D., is co-author of the study.The
study is funded the National Institute of Neurological Disorders and
Stroke (NINDS) of the National Institutes of Health.
"In the
future, we could theoretically treat chronically epileptic patients
with stem cell factors that induce new neuronproduction and see if it
alleviates their learning and memory problems and depression; or we
could prescribe exercise, enriched environment or anti-depressants,"
said Shetty. "All of these treatments are known to considerably
increase adult neurogenesisin the hippocampus where learning, memory
and mood are regulated."
In the Duke study, rats were induced to
have seizures and hippocampal injuryanalogous to humans with temporal
lobe epilepsy – the most common form of epilepsy. Immediately following
the acute seizures, there was a 60 percent increase in new neuron
production in the brain's hippocampus.A respite period with no seizures
lasted for four to six weeks, and then seizures recurred with
increasing severity – the chronic phase of temporal lobe
epilepsy.During the chronic phase,rats displayed an average 75 percent
decrease in neurogenesis compared with normal rats.
The more
frequent the rats' seizures were, the fewer new neurons they produced
in the long term, the study showed. And, the fewer neurons their brains
produced, the more likely they were to suffer more seizures.
"With
chronic epilepsy, the brain's wiring is reorganized to become more
excitable," said Shetty. "The seizures induce changes in nerve cells
that make them more susceptible to additional seizures."
The
rapid production of new nerve cells following acute seizures was
thought to repair damage, said Shetty. But the Duke study, as well as
earlier studies, indicate that such rapid neurogenesis actually
dispatches neurons to the wrong places and contributes to abnormal
brain circuitry and hyper-excitability of neurons. Moreover, the
delicate balance between excitatory neurons that fire signals and
inhibitory neurons which halt them is lost, tipping the balance toward
hyper-excitability.
"Studying early time-points in the epileptic
brain produces an entirely different picture than studying the
long-term effects of chronic seizures," said Shetty. "Understanding the
brain's long-term response to epileptic injury will enhance our ability
to treat the disease," he added.
