Potential
solution for feeding, swallowing difficulties in children with digeorge
syndrome, autism
Ref.
http://www.sciencedaily.com/
Collaborative
research out of the George Washington University (GW) reveals new information
on the pathogenesis of feeding and swallowing difficulties often found in children
with neurodevelopmental disorders, including autism and intellectual
disability. Using an animal model of DiGeorge/22q11 Deletion Syndrome, a
genetic disorder that causes autism and intellectual disability, the GW group
found clear signs of early feeding and swallowing disruption, and underlying
changes in brain development. The research, featured on the cover of Disease
Models & Mechanisms, may even lead to a cure for these difficulties --
known as pediatric dysphagia.
"We found that the same mechanisms causing
neurodevelopmental disorders are disrupting development in parts of the nervous
system that control swallowing and feeding," said Anthony-Samuel LaMantia,
Ph.D., professor of pharmacology and physiology at the GW School of Medicine
and Health Sciences (SMHS) and director of the GW Institute for Neuroscience.
"Cranial nerves, which control food intake and swallowing, aren't
developing correctly, which likely contributes to mis-coordination. This is
good news -- this is something we can fix."
Up to 80 percent of children with developmental disorders have
difficulty ingesting, chewing, or swallowing food, leading to food aspiration,
choking, or life-threatening respiratory infections. Despite its high
co-incidence with developmental disorders, little was previously known about
pediatric dysphagia.
"A lot of children with pediatric dysphagia tend to be
sicker from birth onward. Making the health of these kids as stable as possible
from birth onward would allow clinicians to pick up on developmental signs
sooner, which are often masked by more immediate problems like having ear or
respiratory infections, not sleeping or not gaining weight," said
LaMantia. "The physiological stress caused by the complications of
dysphagia early on likely exacerbates the fundamental behavior issues that will
emerge later. A happy, healthy baby is often able to focus on observing and
gathering information to drive important experience dependent changes in the
brain. A sick baby has less time to do so, possibly making cognitive outcomes
even worse."
These findings were a collaborative effort between LaMantia, and
Sally Moody, Ph.D., professor of anatomy and regenerative biology at SMHS, with
important contributions from Beverly Karpinski, a research scientist who works
jointly with LaMantia and Moody; Thomas Maynard, Ph.D., associate research
professor of pharmacology and physiology at SMHS and director of the GW
Institute for Neuroscience Biomarkers Core; and Irene Zohn, Ph.D. associate
professor of pediatrics and pharmacology and physiology and Investigator in the
Center for Neuroscience Research at Children's National Medical Center.
LaMantia's lab had been working on issues surrounding disrupted
development from DiGeorge/22q11Deletion Syndrome and Moody's lab had, over the
course of her career, been working on issues specific to cranial nerve neurons
and how they relate to the development of peripheral neurons and cranial facial
targets. The combined expertise led to this discovery and will lead to future
collaborations.
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