A new study finds that a component of
aspirin binds to an enzyme called GAPDH, which is believed to play a major role
in neurodegenerative diseases, including Alzheimer's, Parkinson's and
Huntington's diseases.
Researchers at the Boyce Thompson
Institute and John Hopkins University discovered that salicylic acid, the
primary breakdown product of aspirin, binds to GAPDH, thereby stopping it from
moving into a cell's nucleus, where it can trigger the cell's death. The study,
which appears in the journal PLOS ONE, also suggests that derivatives of
salicylic acid may hold promise for treating multiple neurodegenerative
diseases.
Senior author Daniel Klessig, a
professor at Boyce Thompson Institute and Cornell University, has studied the
actions of salicylic acid for many years, but primarily in plants. Salicylic
acid is the critical hormone for regulating the plant immune system. Previous
studies have identified several targets in plants that are affected by
salicylic acid, and many of these targets have equivalents in humans.
In the new study, the researchers
performed high-throughput screens to identify proteins in the human body that
bind to salicylic acid. GAPDH (Glyceraldehyde 3-Phosphate Dehydrogenase) is a
central enzyme in glucose metabolism, but plays additional roles in the cell.
Under oxidative stress--an excess of free radicals and other reactive
compounds--GAPDH is modified and then enters the nucleus of neurons, where it
enhances protein turnover, leading to cell death.
The anti-Parkinson's drug deprenyl
blocks GAPDH's entry into the nucleus and the resulting cell death. The
researchers discovered that salicylic acid also is effective at stopping GAPDH
from moving into the nucleus, thus preventing the cell from dying.
"The enzyme GAPDH, long thought
to function solely in glucose metabolism, is now known to participate in
intracellular signaling," said co-author Solomon Snyder, professor of
neuroscience at Johns Hopkins University in Baltimore. "The new study
establishes that GAPDH is a target for salicylate drugs related to aspirin, and
hence may be relevant to the therapeutic actions of such drugs."
Furthermore, they found that a
natural derivative of salicylic acid from the Chinese medical herb licorice and
a lab-synthesized derivative bind to GAPDH more tightly than salicylic acid.
Both are more effective than salicylic acid at blocking GAPDH's movement into
the nucleus and the resulting cell death.
Earlier this year, Klessig's group
identified another novel target of salicylic acid called HMGB1 (High Mobility
Group Box 1), which causes inflammation and is associated with several
diseases, including arthritis, lupus, sepsis, atherosclerosis and certain
cancers. Low levels of salicylic acid block these pro-inflammatory activities,
and the above mentioned salicylic acid derivatives are 40 to 70 times more
potent than salicylic acid at inhibiting these pro-inflammatory activities.
"A better understanding of how salicylic acid and its
derivatives regulate the activities of GAPDH and HMGB1, coupled with the
discovery of much more potent synthetic and natural derivatives of salicylic
acid, provide great promise for the development of new and better salicylic
acid-based treatments of a wide variety of prevalent, devastating
diseases," said Klessig.
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