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Scientists decipher the formation of lasting
memories
Researchers at Karolinska Institutet have discovered a
mechanism that controls the brain's ability
to create lasting memories. In experiments
on genetically manipulated mice, they were
able to switch on and off the animals'
ability to form lasting memories by adding a
substance to their drinking water. The
findings, which are published in the
scientific journal PNAS, are of potential
significance to the future treatment of
Alzheimer's and stroke.
"We are constantly being swamped with sensory impression,"
says Professor Lars Olson, who led the
study. "After a while, the brain must decide
what's to be stored long term. It's this
mechanism for how the connections between
nerve fibers are altered so as to store
selected memories that we've been able to
describe."
The ability to convert new sensory impressions into lasting
memories in the brain is the basis for all
learning.
Much is known about the first
steps of this process, those that lead to
memories lasting a few hours, whereby
altered signalling between neurons causes a
series of chemical changes in the
connections between nerve fibers, called
synapses.
However, less is understood about
how the chemical changes in the synapses are
converted into lasting memories stored in
the cerebral cortex.
A research team at Karolinska Institutet has now discovered
that signalling via a receptor molecule
called nogo receptor 1 (NgR1) in the nerve
membrane plays a key part in this process.
When nerve cells are activated, the gene for
NgR1 is switched off, and the team suspected
that this inactivation might be important in
the creation of long-term memories.
To test
this hypothesis they created mice with an
extra NgR1 gene that could remain active
even when the normal NgR1 was switched off.
"Doing this, we found that the ability to retain something
in the memory for the first 24 hours was
normal in the genetically modified mice,"
says Professor Olson.
"However, two
different memory tests showed that the mice
had serious difficulties converting their
normal short-term memories to long-term
ones, the kind that last for months."
In order to be able to switch the extra NgR1 gene on and
off, the group attached a regulatory
mechanism to the gene that reacted to a
harmless additive in their drinking water.
When the extra gene was then switched off,
the mice retained their normal ability to
form long-term memories. By subsequently
switching it off at different times after a
memory-forming event, they were able to
pinpoint the effect of the NgR1 gene to the
first week after such an event.
"We know that concussion can cause someone to forget events
that occurred in the week before the injury,
what we call retrograde amnesia, even though
they can remember events that occurred
earlier than about a week before. This we
believe tallies with our findings," says
Alexandra Karlén, one of the scientists
involved in the study.
The scientists hope that their findings will eventually be
of use in the development of new treatments
for memory impairments, such as those
related to Alzheimer's and stroke.
Medicines
designed to target the NgR1 receptor system
would be able to improve the brain's ability
to form long-term memories. The studies were
conducted in collaboration with American
researchers at the National Institute on
Drug Abuse (NIDA), NIH.
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