Scientists find new, inexpensive way to
predict Alzheimer's disease
Your brain's capacity for information is a reliable
predictor of Alzheimer's disease and can be
cheaply and easily tested, according to
scientists.
"We have developed a low-cost behavioral assessment that
can clue someone in to Alzheimer's disease
at its earliest stage," said Michael Wenger,
associate professor of psychology, Penn
State.
"By examining (information) processing capacity, we can
detect changes in the progression of mild
cognitive impairment (MCI)."
MCI is a condition that affects language, memory, and
related mental functions.
It is distinct from the ordinary mental degradation
associated with aging and is a likely
precursor to the more serious Alzheimer's
disease.
Both MCI and Alzheimer's are linked to a steady decline in
the volume of the hippocampus, the area of
the brain responsible for long term memory
and spatial reasoning.
MRIs -- magnetic resonance imaging -- are the most reliable
and direct way to detect hippocampal atrophy
and diagnose MCI. But for many, the
procedure is unavailable or too expensive.
"MRIs can cost hundreds of dollars an hour," Wenger said.
"We created a much cheaper alternative,
based on a memory test, that correlates with
hippocampal degradation."
Wenger and his collaborators at the Mayo Clinic College of
Medicine, Rochester, Minn., detail their
findings in a recent issue of the Journal
of Mathematical Psychology.
From a computer model of an atrophying hippocampus, the
researchers determined how to estimate
capacity with a statistical measure of how
quickly tasks are completed.
Applying this analysis to a memory test for people
with MCI, the researchers were able to gauge
their hippocampal capacity and compare it to
the progression of their ailment.
"My collaborators at the Mayo Clinic backed up this study
with MRIs for the MCI group," Wenger said.
"These capacity measures we developed showed a
reliable relationship to the hippocampal
volume measurements, so we know we are on
the right track."
The scientists began by modeling the hippocampus as a
complex electrical circuit.
Equations governing electric current and voltage
mimicked the electrical firing of neurons
within the circuit. The researchers switched
off neurons in the simulation to model
atrophy of the hippocampus.
With fewer cells available to process electrical signals,
the model hippocampus slowed down, but its
capacity for processing information
decreased at an even faster rate.
Capacity was the most sensitive measure of how the
hippocampus was deteriorating, more than the
average processing speed.
"We then applied this to the gold standard of the field --
the Free and Cued Selective Reminding Test (FCSRT),"
Wenger said.
"This is a test that can discriminate between normal
age-related memory changes and changes
caused by impairment."
The researchers gave this test to five groups of
participants: college students, healthy
middle-aged adults, healthy elderly
individuals, people with diagnosed cases of
MCI, and a control group of age-matched
individuals without MCI.
The first three groups each had 100 members and the last
two each had 50.
During the FCSRT, the researchers showed the participants
descriptive words, such as "part of the
body" and "artery" and asked the
participants to choose the picture that fit
these cues from a set of 24 images, in this
case, a picture of a heart.
The psychologists then asked the subjects to recall as many
items as they could. For objects they failed
to remember, the psychologists provided the
category cues, providing more information
and testing the limits of the subjects'
capacity.
The researchers analyzed the response times for the tasks
and the number of items that were recalled,
with and without additional cues.
The MCI group showed the greatest sensitivity to added cues
– the additional input either substantially
helped or inhibited their performance. But
like the computer model, estimates of
capacity highlighted the greatest cognitive
difference between the MCI group and the
others.
This study's approach to defining processing capacity is
unusual. The scientists combined disparate
principles of engineering and statistics,
mathematically translating processing
capacity into what is called the "hazard
function."
The hazard function is well known in engineering, but
relatively new for fields like psychology.
It gives the probability that a task that is
not yet completed will be completed in the
next interval of time.
By measuring how long it takes a participant to recall the
objects during the FCSRT, the psychologists
fit a model based on the hazard function to
each participant and obtain a measure of his
or her capacity for the memorization task.
The difference in hazard function measures between the MCI
group and all other groups was statistically
much more pronounced than the differences
between all groups in the number of items
they recalled.
These hazard function differences also outweighed the
contrasts between all groups in their
response times.
The hazard function model proved to be the most sensitive
diagnostic for cognitive distinctions in the
groups, making it a reliable indicator of
capacity and a better signal of the
underlying hippocampal atrophy than
processing speed alone.
The researchers' results are valid for every person, not
just for the whole group. Since the modified
FCSRT relies on personal reaction times,
hazard analysis and performance, it can
track the progression of MCI for anyone,
anywhere there is access to a computer.
"These results are still preliminary, but very
encouraging," Wenger said. "We plan to study
what this approach can tell us about mental
impairments related to other conditions,
like iron deficiencies, in the future."
###
Wenger worked with Selamawit Negash, neurology research
fellow, Ronald C. Peterson, professor of
neurology, and Lyndsay Peterson, research
associate, all at the Mayo Clinic College of
Medicine.
The National Institute on
Aging provided funding for this project.
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