Problems
with a key group of enzymes called topoisomerases can have profound
effects on the genetic machinery behind brain development and
potentially lead to autism spectrum disorder, according to research
announced today in the journal Nature. Scientists at the
University of North Carolina School of Medicine have described a finding
that represents a significant advance in the hunt for environmental
factors behind autism and lends new insights into the disorder’s genetic
causes.
“Our study shows the magnitude of what
can happen if topoisomerases are impaired,” said senior study author
Mark Zylka, PhD, associate professor in the Neuroscience Center and the
Department of Cell Biology and Physiology at UNC. “Inhibiting these
enzymes has the potential to profoundly affect neurodevelopment —
perhaps even more so than having a mutation in any one of the genes that
have been linked to autism.”
The study could have important implications for ASD detection and prevention.
“This could point to an environmental
component to autism,” said Zylka. “A temporary exposure to a
topoisomerase inhibitor in utero has the potential to have a
long-lasting effect on the brain, by affecting critical periods of brain
development.”
This study could also explain why some
people with mutations in topoisomerases develop autism and other
neurodevelopmental disorders.
Topiosomerases are enzymes found in all
human cells. Their main function is to untangle DNA when it becomes
overwound, a common occurrence that can interfere with key biological
processes.
Most of the known
topoisomerase-inhibiting chemicals are used as chemotherapy drugs. Zylka
said his team is searching for other compounds that have similar
effects in nerve cells. “If there are additional compounds like this in
the environment, then it becomes important to identify them,” said
Zylka. “That’s really motivating us to move quickly to identify other
drugs or environmental compounds that have similar effects — so that
pregnant women can avoid being exposed to these compounds.”
Zylka and his colleagues stumbled upon
the discovery quite by accident while studying topotecan, a
topoisomerase-inhibiting drug that is used in chemotherapy.
Investigating the drug’s effects in mouse and human-derived nerve cells,
they noticed that the drug tended to interfere with the proper
functioning of genes that were exceptionally long — composed of many DNA
base pairs. The group then made the serendipitous connection that many
autism-linked genes are extremely long.
“That’s when we had the ‘Eureka
moment,’” said Zylka. “We realised that a lot of the genes that were
suppressed were incredibly long autism genes.”
Of the more than 300 genes that are
linked to autism, nearly 50 were suppressed by topotecan. Suppressing
that many genes across the board — even to a small extent — means a
person who is exposed to a topoisomerase inhibitor during brain
development could experience neurological effects equivalent to those
seen in a person who gets ASD because of a single faulty gene.
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