When a key protein needed to generate new brain cells during prenatal and early childhood development is missing, part of the brain goes haywire, researchers say.
That can cause an imbalance in the brain’s circuitry leading to long-term cognitive and movement behaviors characteristic of autism spectrum disorder, according to a new study.
“During brain development, there is a coordinated series of events that have to occur at the right time and the right place in order to establish the appropriate number of cells with the right connections,” says Juan Pablo Zanin, a research associate at Rutgers University-Newark and lead author of a paper in the Journal of Neuroscience.
“Each of these steps is carefully regulated and if any of these steps are not regulated correctly, this can impact behavior.”
Zanin and coauthor Wilma Friedman, professor of cellular neurobiology in the biological sciences department, looked at the protein p75NTR—needed to regulate cell division—to determine its exact function in brain development, gain a better understanding of how this genetic mutation could cause brain cells to die off, and discover whether there is a genetic link to autism or neurological diseases like Alzheimer’s.
Although p75NTR is not a gene specifically linked to autism, researchers place it in a family of proteins needed for brain cells to develop, function, and survive. The exact timing of the expression of this protein during brain development is critical.
“This protein has been examined in regard to neurodegeneration as occurs in Alzheimer’s disease and cell death after brain injury,” says Friedman. “But it has not been looked at regarding the importance it has in generating new neurons.”
Working in the laboratory with genetically engineered mice, the researchers found that mice without the p75NTR protein had more brain cells than should normally exist—causing problems in the cerebellum, the working unit of the brain that regulates movement and balance as well as cognitive function, and one of the key brain regions that autism affects.
For the new study, the researchers trained mice—with and without the p75NTR protein—to associate a quick puff of air with a blinking light. Mice with the protein learned to blink and shut their eyes when they saw the light while mice without the protein did not.
Other scientific studies have found this same learning deficit in mice with mutations in genes associated with autism.
About one in every 59 children in the US currently receives an autism diagnosis, up from one in every 150 in 2000, according to the Centers for Disease Control and Prevention. Although symptoms vary, the disorder causes difficulties in social interactions with others and often results in repetitive behaviors, speech issues, memory problems, and difficulties in understanding nonverbal cues.
While scientists have no clear answer as to the consequences of a brain with too many neurons, autism, primarily a genetic disease, has been associated with an unusually large brain size. Some scientists think that early brain overgrowth could be a marker for the disorder.
“It is important to understand how the brain’s circuitry is built and how it regulates behavior normally,” Friedman says. “This research shows us that when it is not generated properly it is going to have an impact on many behaviors.”
Source: Rutgers University