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How
Stress
Can
Lead to Alzheimers & Parkinson’s Disease
In 2007
Nobel Prize winner James Watson came face-to-face with the chemical
structure he once helped to unravel in a very personal way.
However, there was one
small stretch of DNA on chromosome 19, that he chose to leave in the
dark 50 years after solving the puzzle of DNA…..That region was the
area that codes for the apolipoprotein E (APOE) gene. Since
the early
1990s APOE has been a telling genetic marker of Alzheimer’s risk:
certain forms
of it correlate strongly with the development of the disease. Watson’s
grandmother
suffered from Alzheimer’s, but without any reasonable treatments or
proved
preventive strategies, the discoverer of the double helix decided the
information
was too volatile, its revelation creating more potential
harm than good. So he decided to keep it
secret.
Watson’s
a pprehension could be
classed as understandable: treatments for Alzheimer’s have
consistently
failed. However as scientists learn more and more about the brain,
they have come to realise that genetics alone rarely dictates the course of an
illness. Instead brain disorders result from a complex interaction
between our
genes and the environments to which we are exposed. Indeed, a set of
recent
studies has just uncovered an important environmental instigator of
neurodegenerative
disease:
stress.
Tight Quarters
Since Alois
Alzheimer first documented “presenile dementia” in a patient at the
beginning
of the 20th century, doctors have often observed that the disease runs
in
families. But not until the early 1990s, about the same time the APOE
link surfaced,
did researchers glean hints that nongenetic factors contribute to it.
 Epidemiologist Brenda
Plassman of Duke University teased out this
environmental effect by studying identical twins, who share virtually
the same
genetic material. If a disease is driven purely by genetics, then when
one twin
develops it, the other will be stricken as well. By analysing data from
a large
cohort of identical twins (all of them male veterans of World War II),
Plassman
reported in 2000 that when one twin developed Alzheimer’s, the other
twin
developed the disease only
40 percent
of the time. Concluding that factors besides genetics must be at play,
the
investigators have since been searching for those contributors. Among
the possibilities:
subtle medical conditions, occupational characteristics and physical
activity
levels.
Of
course, your job and the amount you exercise both have an effect on
your level
of psychological stress, the mind and body’s response to challenge and
change.
But only this year did evidence suggest that stress might be a key
ingredient
in the recipe for cognitive decline. To explore how different
environments
might affect the development of Alzheimer’s, neuroscientist Mark
Tuszynski and
his colleagues examined the brains of aged rhesus monkeys that had
spent their
early lives in either small or standard-size cages. Tight quarters have
been
shown to stress these animals, elevating levels of glucocorticoid
hormones in
their blood. The exact cause of this hormonal rise—whether it comes
from a
feeling of being trapped or an inability to get adequate exercise, or
both—is
still an open question. Cortisol, a glucocorticoid hormone released when humans
experience stress, influences the brain through specialised molecular
receptors
on neurons in a number of brain regions. When cortisol binds to its
receptor,
the interaction triggers molecular events that reduce communication at
synapses,
the junctions between neurons, w hich may ultimately cause the
connections to
wither away. Using protein
stains that adhere specifically to synapses,
enabling them to be seen, Tuszynski’s team determined the relative number of
synapses in all the monkeys. Using a similar method, the researchers
also
assessed the amount of sticky amyloid plaques, a pathological hallmark
of
Alzheimer’s.
 Compared with the monkeys raised in
standard-size
cages, those that lived in smaller cages had, on average, a
significantly
higher density of plaques and fewer synapses in one part of their
brain—the
same pattern seen in the brains of Alzheimer’s patients at autopsy. The
finding
suggests that the size of an animal’s cage—and perhaps the amount of
stress it
endures as a result—may shape that animal’s brain in a way that affects
its
vulnerability to certain types of degeneration as it ages.
Interestingly, the
amount of plaque riddling the brains of the monkeys housed in smaller
cages varied
a lot, indicating that stress affects individuals differently. After
all, we
all know people who seem to take even mildly negative events to heart
as well
as others in similar situations who take their plight in stride.
The
evidence from Tuszynski’s group has its limitations. Observations in
monkeys
living in labs do not precisely mirror the human condition (well,
maybe, this
doesn’t say much for us scientists who ‘live in labs’….!). In addition,
these
findings correlate only one aspect of early-life experience with
pathological
signs of degeneration. We do not know that the stress caused the
changes, nor
do we know whether those changes resulted in true cognitive slipups,
because
the scientists could not test the animals’ cognitive function.
Toxic Tension
Nevertheless,
additional
studies
in rodents suggest that even intermittent strain can tip the
scales toward dementia, even if it does not lead to cognitive breaks on
its own.
In March 2010 neuropharmacologist Karim Alkadhi of the University of
Houston and
his colleagues put rats at risk for dementia by injecting them with
very low
concentrations of beta-amyloid peptides, the molecules that form
plaques in
humans. (see picture below) The researchers then stressed some of the
animals by placing an
intruder rat in their home cage. As expected, blood levels of
corticosterone, a
glucocorticoid, rose in the stressed rats.
 Then the scientists
placed each rat in a water tank
containing a maze. A rat had to find the path that led to a platform to
escape
the water—a rodent test of learning and memory. Usually after a few
tries, a
rat will remember the correct route; it will then swim directly to the
platform, even a day or two later. Most of the experimental
rats—including
those that had been given amyloid injections and those forced to face
intruders—performed well. The rats that had received both the shots and
the
unwanted visitor, however, had difficulty. So although stress alone
does not
degrade memory, it does seem to push at-risk animals over the edge,
making them
less able to learn and remember new things.
Other
work hints that stress may hasten the onset of Parkinson’s disease, a
neurodegenerative disorder characterized by motor difficulties rather
than
cognitive deficits. The loss of brain cells that produce dopamine, a
neurotransmitter essential for voluntary movement, causes Parkinson’s
patients
to shake, become rigid and lose coordination.
To
re-create these deficits in rats, behavioral neuroscientist Gerlinde
Metz
infused a toxic drug into a brain area rich with dopamine neurons. Some
of
these animals were put into a Plexiglas tube for 20 minutes a day for
two
weeks, producing a temporary boost in stress hormone levels. Another
group
received corticosterone shots, which kept the animals’ stress hormones
high
throughout the experiment. Metz’s team then tested the motor skills of
all the
animals. In one exercise, for example, the rats had to slip their paws
through
a narrow opening in a Plexiglas box to extract a small food pellet, an
action
that requires precise and careful movements.
The
Metz team’s toxic treatment is transient; usually the treated rats’
motor
skills improve with time. But the animals with elevated corticosterone
levels—both the ones that spent time in a stressful environment and
those that
received hormone shots— continued to struggle with the pellet
extraction task
long after the other animals had recovered. The results suggest that
stress
impedes the ability of dopamine cells to recover from insults,
triggering or
aggravating Parkinson’s symptoms.
Indelible Mark
Using
such eye-opening studies as these, scientists are learning that stress
is more
than a fleeting emotional setback. Rather, in certain situations,
stress can
leave an indelible mark on our brain.
But
there is good news, too. Stress is a contributor
to neurodegeneration that can be controlled. Just as many individuals
with high
cholesterol levels now take preemptive action to stave off heart
disease, one
day people may use, say, their APOE status to motivate them to adjust
their
lifestyles. Evidence suggests that simple interventions such as
exercise,
meditation and getting enough sleep can help reduce the stress of
life’s encounters.
Such measures might even ease the anxiety of knowing which APOE stamp adorns
your genome.
References
◆ Acute Stress Modulates Genotype Effects
on
Amygdala Processing in Humans. Helena cousijn et al. in Proceedings of
the
National Acade- my of Sciences uSA, vol. 107, no. 21, pages 9867–9872; may 25,
2010. www.pnas.org/content/107/21/9867.full
◆ Association of Early Experience with
Neurodegeneration in Aged Primates. david a. merrill et al. in
Neurobiology of
Aging, vol. 32, no. 1, pages 151–156; January 2011.
◆ Strain on the
Brain A stressful life may fuel Alzheimer’s and Parkinson’s disease By
Brian
Mossop pages 60-63. Scientific American Mind Volume 22, Number 3,
July/August
2011.
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