As a mom who has a kiddo with epilepsy this article really hit me. I know there's a connection for so many of us, but I may never know what came first the epilepsy or autism. So many questions, still not enough answers.
Preventing autism after epilepsy
Published: Wednesday,
May. 2, 2012 - 2:06 pm
BOSTON, May 2, 2012 -- Basis for the
epilepsy-autism connection is found – and may be reversible with an existing
drug
BOSTON, May 2, 2012 /PRNewswire-USNewswire/
-- Early-life seizures are known to be associated with autism, and studies
indicate that about 40 percent of patients with autism also have epilepsy. A
study from Boston Children's Hospital finds a reason
for the link, and suggests that an existing drug, already shown to be safe in
children, could help prevent autism from developing in newborns who have
seizures.
Led by Frances Jensen, MD, in
the Department of Neurology and
the F.M. Kirby Neurobiology Center at
Boston Children's Hospital, the study suggests that seizures over-activate a
biochemical pathway previously linked to autism, known as the mTOR pathway, and
that this alters the fast-forming circuitry in infants' developing
brains.
In a rat model, Jensen and colleagues showed
that early seizures not only resulted in epilepsy later in life, but also
produced autistic-like behavior. They further showed that disabling the mTOR
pathway – by giving the drug rapamycin before
and after seizures – prevented development of abnormal patterns of connections
(synapses) between brain cells, reduced later-life seizures and eased
autistic-like symptoms.
Findings were published May 2 in the online
journal PLoS ONE.
"In children, there is overlap between
epilepsy and autism, and epilepsy early in life has been linked to later
autism," says Jensen of Boston Children's Hospital. "Our findings
show one of probably many pathways that are involved in this overlap –
importantly, one that is already a therapeutic target and where treatment can
reverse the later outcome."
Specifically, the study demonstrated that a
group of signaling molecules, known collectively as the mTOR pathway, shows
increased activation after a seizure. This increased signaling – above and
beyond the surge that normally occurs early in life – disrupted the normal
balance of synapse and circuit development to produce epilepsy and altered
social behavior. Rapamycin treatment inhibited mTOR signaling, reducing
susceptibility to seizures and preventing seizure-induced changes in the
synapses.
The study uncovers a new link whereby epilepsy
and autism may interact in early development. Last December, Jensen and
colleagues published a related study finding
that seizures exaggerated excitation and synaptic strengthening too soon in a
rat model, causing synapses to lose their plasticity -- their ability to
reconfigure in response to input from the outside world. When they gave the
rats a drug called NBQX, which blocks receptors associated with excitation,
these problems were reversed.
The mTOR pathway is already known to be
over-active in tuberous sclerosis complex (TSC)
a genetic disorder treated at Boston Children's that often includes epilepsy
and autism. The hospital is currently conducting a clinical trial of
rapamycin in children with TSC.
"Our study suggests that even without
tuberous sclerosis, seizures are inducing the mTOR pathway, and might on their
own be contributing to the development of autism," says Jensen. "It
appears that blocking the mTOR pathway briefly after the initial seizures may
reduce the risk of later epilepsy and autism. This research also suggests
that the fields of epilepsy and autism may inform each other about new
treatment targets."
For further background, see this feature published
last year in Nature Medicine.
Delia Talos, PhD, Hongyu Sun, MD, PhD, and
Xiangping Zhou, MD, PhD, all of the Department of Neurology and Division of
Neuroscience at Boston Children's Hospital, shared first authorship on the
paper. The study was funded by the National Institutes of Health, the
National Institute ofChild Health and Human
Development, the Tuberous Sclerosis Alliance, the Ruth L.
Kirschstein National Research Service Award and the Canadian Institutes of Health
Research.
Boston Children's Hospital is
home to the world's largest research enterprise based at a pediatric medical
center, where its discoveries have benefited both children and adults since
1869. More than 1,100 scientists, including nine members of the National Academy of Sciences, 11 members of the
Institute of Medicine and nine members of the Howard Hughes Medical Institute
comprise Boston Children's research community. Founded as a 20-bed hospital for
children, Boston Children's today is a 395 bed comprehensive center for
pediatric and adolescent health care grounded in the values of excellence in
patient care and sensitivity to the complex needs and diversity of children and
families. Boston Children's also is the primary pediatric teaching affiliate of Harvard Medical School. For more information about
research and clinical innovation at Boston Children's, visit: http://vectorblog.org.
CONTACT: Meghan
Weber Boston Children's Hospital 617-919-3110meghan.weber@childrens.harvard.edu
SOURCE Boston Children's Hospital
Read more here: http://www.sacbee.com/2012/05/02/4460761/preventing-autism-after-epilepsy.html#storylink=cpy
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