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Enzyme fights Mutated Protein in inherited
Parkinson’s Disease
Newswise — An enzyme that naturally occurs
in the brain helps destroy the mutated
protein that is the most common cause of
inherited Parkinson’s disease, researchers
at UT Southwestern Medical Center have
found.
Their study, using human cells, provides a
focus for further research into halting the
action of the mutated protein. One of the
most famous carriers of the mutation is
Google co-founder Sergey Brin, who wrote
about it on his blog in 2008.
“There are currently enormous efforts to
identify potential therapies based on
inhibiting this mutated protein,” said Dr.
Matthew Goldberg, assistant professor of
neurology and psychiatry and senior author
of the paper, which appears online in the
journal Public Library of Science.
“Our paper is a major advance because we
identify a protein that binds to the mutated
protein and promotes its breakdown,” he
said.
The particular mutation that they studied
affects a protein whose function is not well
understood. In its normal form, it appears
to have multiple sites where other molecules
can attach themselves, like a space station
with many docking areas.
Several mutations can affect the protein,
which is named LRRK2. Some of the mutations
cause Parkinson’s disease.
The current theory is that the mutation
leads to increased function of LRRK2 and to
the formation of abnormal clumps of proteins
inside brain nerve cells. The cells
eventually die from these effects.
In the current study, the researchers used
cultured human kidney cells and found that
LRRK2 and a protein called CHIP “robustly”
associated with each other.
Further testing showed that CHIP and LRRK2
could bind to each other in two different
ways, either directly or indirectly by a
third molecule that acted as a bridge.
When CHIP bound to either the normal or
mutant form of LRRK2, levels of LRRK2 in the
cell decreased, the researchers found. This
occurred because the cells increased the
rate at which they destroyed LRRK2.
“CHIP may be a useful therapeutic target for
treatments to break down LRRK2 in people
with Parkinson’s,” Dr. Goldberg said.
“Our next step is to identify cellular
mechanisms that signal LRRK2 to be degraded
by CHIP or by other mechanisms,” he said.
“Because LRRK2 mutations are believed to
cause Parkinsonism by increasing the
activity of LRRK2, enhancing the normal
mechanisms that target LRRK2 for degradation
by CHIP may be therapeutically beneficial.”
Lead author Xiaodong Ding, senior research
associate in neurology at UT Southwestern,
also contributed to the study.
The study was funded in part by the David M.
Crowley Foundation.
Visit
www.utsouthwestern.org/neurosciences
to learn more about UT Southwestern’s
clinical services in the neurosciences.
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