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Common Cell-Nucleus Receptor is Key Component
of Internal Clock
Molecule's Sensitivity to Lithium Points to New Therapies
for Bipolar, Circadian Rhythm Disorders
(Philadelphia, PA) - Researchers at the University
of Pennsylvania School of Medicine discovered that a key receptor
protein is a critical component of the internal molecular clock in mammals.
What’s more, this molecule - called Rev-erb - is sensitive to lithium
and may help shed light on circadian rhythm disorders, including bipolar
disorder. The findings, which also provide insight into clock-controlled
aspects of metabolism, are reported in this week’s issue of Science.
“We’re interested in the internal control of metabolism because
feeding behavior is on a daily cycle, and hormonal activities that regulate
this are circadian,” says senior author Mitch Lazar, MD,
PhD, Director of the Institute for Diabetes, Obesity, and Metabolism
at Penn. “Many studies, including those here at Penn, suggest a
relationship between the human circadian clock and metabolism. Proteins
are the gears of the clock, and not much is known about what regulates
protein levels within the cell.”
Rev-erb was known to be a key component of the clock that exists in most
cells of the body. Rev-erb inhibits clock genes called bmal and
clock, but within a normal 24-hour circadian cycle the Rev-erb
protein is destroyed within the cell, allowing bmal and other clock proteins
to increase. Among other actions, these clock genes cause Rev-erb to increase,
which again inhibits bmal and clock. “The time
it takes for that to happen determines the length of the cycle-roughly
24 hours-and keeps the clock going,” explains Lazar.
Penn colleague and coauthor Peter Klein, MD, PhD, Assistant
Professor of Medicine, discovered a few years ago that the drug lithium,
used to treat biopolar illness, inhibits GSK3, an enzyme known to regulate
circadian rhythm in several animal species. In the present study, the
researchers showed that the destruction of Rev-erb, a receptor shown previously
by Lazar and others to play a role in maintaining normal metabolism, is
prevented by GSK3 in mouse and human cells. “It’s like pulling
a pin out of the gears of the clock, to allow them to turn in a synchronized
manner,” says Lazar.
Lithium blocks this action of GSK3, tagging Rev-erb for destruction, which
leads to activation of clock genes such as bmal1. “We suggest
that just as our cells in the incubator need to have their internal clocks
reset, maybe this is what happens in some people with circadian disorders,”
says Lazar. “One effect of lithium may be to reset clocks that become
stuck when Rev-erb levels build up.”
These results point to Rev-erb as a lithium-sensitive component of the
human clock and therefore a possible target for developing new circadian-disorder
drugs. Some patients taking lithium have developed kidney toxicity and
other problems. Lazar surmises that new treatments that lead to the destruction
of Rev-erb would have the potential of providing another point of entry
into the circadian pathway.
Noting that Rev-erb is present in metabolically active tissues, Lazar
and his team at the Institute for Diabetes, Obesity, and Metabolism are
also interested in the relationship between the control of the circadian
clock and metabolic diseases such as obesity and diabetes. “There
is a dynamic interplay between circadian rhythms and metabolism,”
Lazar says. “You don't eat while you are sleeping, and the body
needs to take this into account.”
Study co-authors are Lei Yin and Jing Wang, both from Penn. The research
was funded by the National Institute of Diabetes & Digestive &
Kidney Diseases and the National Institute of Mental Health.
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