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BIOMARKER FOR PTSD AND WHY PTSD IS SO
DIFFICULT TO
TREAT -- PTSD is the most common mental health
disorder
among veterans of the conflicts in Afghanistan
and Iraq.
As the profile of PTSD rises, new findings are
increasing researchers' understanding.
For more about PTSD, use the VA Watchdog search
engine...click here...
http://www.yourvabenefits.org/sessearch.php?q=ptsd&op=and
Story here...
http://www.sciencedaily.com/releases/2007/11/071107211450.htm
Story below:
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-------------------------
Biomarker For PTSD And Why PTSD Is So Difficult
To Treat
ScienceDaily -- New research identifies a characteristic physiological
response in veterans with post-traumatic stress disorder (PTSD) that could
be used as a biomarker to diagnose the disease. Other findings show how
trauma disables normal brain functioning and highlight deficits in basic
mechanisms of learning and memory. Recent findings also show that a common
neurological basis explains altered emotional responses in veterans with
PTSD, and that fear learning caused by trauma is different from other
types and may explain why it is more difficult to treat.
"PTSD can be a debilitating disorder that creates cognitive disability as
well as internal stress for the victim and produces stress for family and
friends. And it is an increasing public health concern," says Bruce
McEwen, PhD, of Rockefeller University in New York City. "Understanding
what goes on in the brain is critical to finding successful treatments,
including pharmaceutical therapies and cognitive behavioral therapies that
enhance extinction of the fear-related memories."
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PTSD is the most common mental health disorder
among veterans of the conflicts in Afghanistan and Iraq. As the profile of
PTSD rises, new findings are increasing researchers' understanding of the
way memory malfunctions in PTSD, creating characteristic symptoms such as
flashbacks and fear reactions to trigger sounds, even in safe situations.
The disorder is characterized by flashbacks, emotional numbness, and
insomnia. It can result from a catastrophic and threatening event -- a
natural disaster, wartime situation, accident, domestic abuse, or violent
crime. Symptoms usually develop within three months, but can emerge years
after the initial trauma. Estimates indicate more than 7.5 million
American adults have the disorder, according to the National Institute of
Mental Health.
New research with veterans from the Serbo-Croatian War of the early 1990s
confirms previous research showing that veterans with PTSD react in fear
even when shown signals they have come to associate with safety. It also
has led to the identification of the first biomarker for PTSD, which may
become useful in testing the value of treatments for the disorder.
"One of the central features of the disorder is the inability of the brain
to distinguish between dangerous and safe situations," says Michael Davis,
PhD, of Emory University School of Medicine. "For example, a woman who was
raped by a stranger may later not even feel safe with her husband. That
is, she has lost the ability to distinguish between dangerous and safe
situations." Davis will be presenting a special lecture at Neuroscience
2007 titled "Neural Mechanisms of Fear Extinction: Implications for
Psychotherapy."
Working with 33 veterans, Davis measured the degree to which subjects were
startled, as well as their ability to overcome this fear response, as he
evoked certain conditioned responses. He was assisted by Erica Duncan, MD,
and Tanja Jovanovic, PhD, in this research. The study used yellow, green,
and blue lights, which, in pairs, signaled caution or safety. Davis first
trained the subjects to associate the yellow and green lights with a blast
of air to the throat. How hard the veterans blinked was recorded as a
measure of their startle response to this combination of colored lights.
The study then created an association between a blue-green pairing of
lights and no air blast, establishing a signal for relative safety.
To measure how safe the blue light made the subjects feel, Davis then
recorded responses to a blue-yellow signal. What he found was that
although healthy subjects startled less when they saw the blue and yellow
lights than when they saw the green-yellow combination, those with PTSD
could not suppress their fear response. This indicated an inability to
respond to indicators of safety.
"This test can provide a more objective way of measuring fear control
mechanisms that work in healthy people and do not work in patients with
PTSD," says Davis. "In fact, this finding may provide one of the first
biomarkers for PTSD, namely an objective physiological measure of abnormal
fear regulation. It may also become a valuable clinical tool to assess and
compare the effectiveness of different treatments in different populations
of PTSD patients, such as civilians and combat veterans."
Researchers also are moving closer to an answer to the question of what
causes combat-related PTSD, which develops in an estimated 12 percent of
veterans returning from the current conflicts in Afghanistan and Iraq. A
recent study reveals how a combat event can impair subsequent brain
functioning. Although people with PTSD can temporarily learn to extinguish
fear, they are unable to retain this ability.
Working with 14 pairs of identical twins from the Veterans
Administration's Vietnam era twin registry, Mohammed Milad, PhD, at
Boston's Massachusetts General Hospital and Harvard Medical School,
developed a two-day fear conditioning protocol. In each pair of twins,
only one had experienced combat; half of these veterans also had PTSD. On
the first day, the subjects learned to associate a light with a mild
shock. After several trials in which Milad displayed the light without
administering the shock, he found that all groups of subjects were
successful at disassociating the light from their fear of being shocked.
The following day, Milad recorded electrical resistance on the subjects'
skin as a measure of their emotional response to the light. In contrast to
the day before, subjects with PTSD showed a strong fear reaction to the
light. Twins of the PTSD veterans as well as the other combat veterans and
their twins all remained able to inhibit their fear.
"The inappropriate and long-lasting fear observed in PTSD has led
investigators to hypothesize that PTSD patients are unable to inhibit or
extinguish their conditioned fear responses," says Milad. "Our
demonstration that extinction memory is deficient in PTSD veterans but
intact in their noncombat co-twins suggests that the trauma itself caused
this dysfunction.
"These findings argue against the possibility that the ability to control
fear in PTSD patients had already been frail prior to the trauma due to
genetic or environmental factors," he says. To further examine the
biological basis for learning and extinguishing fear in the brain, Milad
plans studies with twins using functional magnetic resonance imaging (fMRI).
More than just mechanisms for fear-related memory may go awry in the
brains of people with PTSD, according to findings by Dutch researchers who
show that learning unrelated to trauma also is affected.
"These neurobiological alterations witnessed in veterans with PTSD provide
some acknowledgement that the problems experienced by them are not just
figments of the imagination but very real neurobiological consequences of
traumatic stress. It is this neurobiological war within that we should
learn to wage and win," says Elbert Geuze, PhD, at the Military Mental
Health Research Center in Utrecht, The Netherlands.
Using fMRI to monitor the brains of 24 male veterans, half with PTSD,
Geuze zeroed in on the neural correlates of memory processing. The
veterans in each group were matched so that pairs were approximately the
same age, and had been deployed at the same time and to the same area.
Geuze first asked the veterans to memorize 12 pairs of words, which were
neutral in terms of emotional content: stone and car, for example, or rose
and house. Later, they were tested on their recall of the word pairs:
Given "stone," they were asked to recall "car."
Compared with veterans without PTSD, those showing symptoms of the
disorder had less activity in the frontal cortex and an overactive
temporal cortex while learning and memorizing the word pairs. "Apparently
patients are unable to fully recruit their frontal cortex, an area
important for working memory processing," Geuze says.
When asked to recall the word pairs, they showed decreased activity in the
brain's right frontal cortex, bilateral middle temporal gyri, and left
hippocampus and parahippocampal gyrus. "Patients seem to use a wrong part
of the brain-the superior temporal cortex instead of the medial temporal
cortex, where the hippocampus is-to perform this task," he says. The
frontal cortex, temporal cortex, and hippocampus all have critical roles
in the basic cognitive processes of learning and memory. The hippocampus,
for example, helps store newly created memories and is connected to areas
of the brain responsible for thinking and language.
"These data support the long-held notion that altered activity in fronto-temporal
circuits of the brain is related to deficits in memory performance in
veterans with PTSD," Geuze says.
Another study examining learning among veterans with PTSD found that three
different physical responses may all be responding to signals from the
same areas of the brain, known to be involved in processing emotional
material. Previous studies have shown these same areas of the brain areas
are dysfunctional in PTSD.
A research team headed by D.A. Powell, PhD, of the Dorn Veterans
Administration Medical Center in Columbia, S.C., worked with nearly 50
veterans, categorized in three groups: healthy veterans, with combat
experience and without, and combat veterans with PTSD. The study involved
a number of trials in which the subjects learned to associate a warning
light and tone with a puff of air directed at their eyes. The warning
signal was displayed five seconds before the tone, which sounded almost
simultaneously with the puff of air.
When the PTSD combat veterans were shown the light after a few trials,
Powell's research team found that the veterans' heart rate accelerated.
The typical response to a sign of potential danger is for the heart to
slow down. And this, in fact, is what the team found among both groups of
veterans without PTSD.
It is also typical for subjects to blink in defense when their eyes are
hit with a puff of air; this defensive eyeblink response is known to
decrease over time, a process known as habituation. The researchers found
that for PTSD veterans, the defensive eyeblink became habituated much
faster than for the study's other subjects, in reaction both to the tone
and to the actual puff of air.
"In other words, hyper-responsivity to a warning signal and hypo-responsivity
to actual aversive stimulation may be a characteristic of combat veterans
with PTSD," says J.P. Ginsberg, a member of the research team.
Additional tests in the study assessed subjects' short-term memory for
verbal information and indicated that the ability to pay attention was
disturbed in those with PTSD. Ginsberg and his colleagues found that
deficits in PTSD combat veterans' ability to memorize new verbal
information correlated to their rapid habituation, a result that links
impairments in physiological and cognitive function as a result of the
disorder.
"We may be able to relate these findings to central nervous system
circuits involving the amygdala, cingulate cortex, and medial prefrontal
cortex, all of which are known to be involved in brain processing of
emotional material and which have been demonstrated to be dysfunctional in
PTSD," says Ginsberg. He notes the same brain regions are involved in
associative learning, physiological regulation of the heart, and attention
to verbal information.
Animal research is aiming to advance the development of effective
therapies for PTSD, and new findings based on studies with rats reveal how
PTSD differs from other anxiety disorders -- and therefore why it can
prove so hard to treat.
Michael Fanselow, PhD, at the University of California, Los Angeles, has
developed a rat model using a regimen he calls stress-enhanced fear
learning. He used this model to examine the way traumatic stress affects
the capacity to learn and remember fear and to test proposed treatment
approaches that focus on the timing and intensity of therapy.
Initially, the rats were placed in a room (A) and given a shock to the
foot. The next day, in a separate setting (B), 15 shocks were administered
over a 90-minute period, a traumatic level of stress. The rats were
returned to the same room for 30 minutes on five subsequent days, but not
exposed to shock. On the sixth day, the rats were placed in a third room
(C), where again they received a single shock to the foot.
Tested in the two rooms in which they received the single shock, the rats
acted far more fearful in setting C. "These findings indicate that fear
learning that occurs after traumatic stress is markedly different from
fear learning that occurs in other circumstances," Fanselow says.
The second part of the study tested the effectiveness of potential
therapies focused on enhancing the extinction of terrifying memories.
Using a method known as massed extinction, in which five 30-minute
extinction sessions were held with five-minute intervals in between,
Fanselow compared the effectiveness of the technique when administered 10
minutes and 72 hours after the traumatic event.
"Recent fear conditioning research suggests that massed extinction or
extinction that starts immediately after conditioning may be especially
effective at fear reduction," Fanselow says.
Once the mass extinction trial was finished, the rats received another
single shock to the foot; their fear response was tested a day later. The
rats treated with mass extinction were compared with an untreated group
and one that had not been exposed to traumatic stress. All three groups
with experience of traumatic stress responded similarly, suggesting that
the massed extinction technique -- whether administered immediately after
trauma or after an initial delay -- is not an effective treatment for
PTSD.
The finding that stress-enhanced fear learning is not changed by various
extinction methods, Fanselow notes, "may begin to explain why PTSD is so
difficult to treat."
"Pavlovian fear conditioning is used in many animal models of fear
learning and memory," says Fanselow. "These animal models have been very
successful at helping to understand the nature of anxiety disorders and
have furthered knowledge such that it has benefited human research on
course and treatment.
"In the case of animal models of PTSD, however, we propose that the
stress-enhanced fear learning model produces symptoms more similar to
those found in PTSD than other animal models."
Adapted from materials provided by Society for Neuroscience.
-------------------------
Larry Scott --
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