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FOR
IMMEDIATE RELEASE
12/15/03
CONTACT: Gordon Mitchell, (608) 263-9826, mitchell@svm.vetmed.wisc.edu; Tracy
Baker-Herman, (608) 263-5013, bakert@svm.vetmed.wisc.edu
RESEARCHERS IDENTIFY
KEY PLAYER IN RESPIRATORY MEMORY MADISON - By studying the "memory" of the
respiratory system, a group of researchers from the University of Wisconsin-Madison
has identified a key player - a protein called BDNF that's involved in learning
- responsible for the body's ability to keep breathing properly, despite
the challenges it may face. The findings, published Dec. 14 in the online
edition of Nature Neuroscience, could provide ideas of new drug targets,
which could lead to new treatments for or ways to prevent a number of potentially
fatal breathing disorders, including sleep apnea, sudden infant death syndrome
and some related to spinal cord injuries, according to the researchers. Every
few seconds, we draw a breath and then release it. If for some reason this
routine is interrupted - oxygen levels are low or airways are blocked, for
example - our bodies respond accordingly. In the case of oxygen deprivation,
the nerve cells in the brain send messages to motor neurons along the spine,
which then tell certain muscles involved in breathing to work harder. As
a result, a person may take deeper breaths. If the breathing disruption is
experienced regularly, the respiratory system remembers the disruption and
most likely will respond more vigorously in the future. Researchers call
this change in neural behavior "neuro-plasticity." In some cases, however,
the respiratory system may not remember, says Gordon Mitchell, chair of the
comparative biosciences department at UW-Madison's School of Veterinary Medicine
and senior author of the recent paper. He notes that some people who have
sleep apnea - a disorder where breathing stops repeatedly during sleep -
may have inadequate respiratory memories. He adds that individuals with spinal
cord injuries in the neck often must rely on ventilators to help them breathe. "For
them, breathing is a bigger problem than never walking again," says Mitchell. "To
breathe is to live." To allow such patients to breathe more easily, Mitchell
and others are exploring the mechanisms underlying respiratory memory so
as to find ways to enhance it, such as through drugs.
"If we can understand how breathing changes as a result of experience, we can
develop techniques to intervene when breathing is compromised," says Tracy Baker-Herman,
a postdoctoral fellow at UW-Madison and first author of the paper. To begin to
uncover these mechanisms, the researchers exposed rats to three five-minute intervals
of hypoxia, or decreased oxygen. Sixty minutes after exposure, they recorded
the respiratory-related activity levels in the phrenic nerve, which controls
the diaphragm muscle. If the activity levels increased after exposure, the researchers
would know that the respiratory system, specifically this nerve, had developed
a memory of low oxygen. The Wisconsin scientists did, in fact, record this memory:
Activity levels after exposure were 80 percent higher than before the intervals
started, suggesting that this nerve remembered experiencing periods of low oxygen
levels, says Mitchell. Making this connection, however, was not enough, says
Baker-Herman. The researchers wanted to know what caused this memory. So, they
analyzed segments of spinal cord taken from rats after they had been exposed
for 60 minutes to either normal or decreased amounts of oxygen. The researchers
looked specifically for changes in the BDNF protein, or brain derived neurotrophic
factor, which is known to sustain and even stimulate neuronal function in the
brain. The findings show that intermittent periods of decreased oxygen increased
concentrations of the BDNF protein in the phrenic nerve by 56 percent. Through
further testing, the researchers learned that BDNF is, in fact, responsible for
increasing activity in this nerve, thereby stimulating a respiratory memory.
For example, when the researchers blocked BDNF production in rats with a new
technique known as RNA interference and then exposed the rats to intervals of
decreased oxygen, they observed no increase in nerve activity. But, when they
injected the protein directly into the phrenic nerve of rats they found that
neuronal activity increased by 125 percent. Both findings, says Mitchell, point
to the integral role BDNF plays in enhancing the respiratory system's response
to disruptions in breathing. "They show causality between BDNF and phrenic long-term
facilitation (or memory)," he says, adding, "the role of BDNF in respiratory
plasticity was not known at all before now." With this new information, Mitchell,
Baker-Herman and others in their group continue to search for additional players
in respiratory memory. "The closer we get to the ultimate cause," says Mitchell, "the
better the chance of developing new pharmaceutical therapies." These therapies
would have the potential not only to restore breathing ability to individuals
struck with devastating spinal cord injuries, but also to alleviate the effects
of sleep apnea - tiredness, learning impairments, high blood pressure, even death
- among the 5 percent of the population with this breathing disorder. Mitchell
adds, "The promise for treating other disorders where breathing is disrupted,
including sudden infant death syndrome and ALS (Amyotrophic Lateral Sclerosis
or Lou Gehrig's disease) is not trivial." But he cautions that the basic science
behind these disorders is still being learned and that pharmacological treatments
will follow only after that knowledge has been gained.
-- Emily Carlson (608)
262-9772, emilycarlson@wisc.edu
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