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FOR IMMEDIATE RELEASE: 10 NOVEMBER 2000
Princeton University
http://www.princeton.edu/ Instant replay: study finds potential mechanism for building long-term memory Princeton scientists have discovered a key mechanism the brain uses to transfer
short-term memories into permanent storage, a finding that could have broad
implications for understanding how the brain maintains long-term stability. Researchers led by neuroscientist Joe Tsien found that the brain appears to
have a system of repeatedly replaying and reinforcing the same cellular event
that led to the initial formation of a memory. The reinforcement is critical
for creating the cell-to-cell connections that constitute long-term memories,
the researchers found. "It's really surprising to find out we need to reactivate this initial learning
event," said Tsien. "It's like learning something again in your brain, only
this time it's due to some kind of spontaneous reactivation mechanism." This observation could yield insights into the much broader question of how the
brain maintains a continuity of knowledge and memories over a lifetime despite
the constant turnover of molecules and proteins. The insight also may one day help with the understanding of human diseases such
as schizophrenia, said Tsien. If the process of consolidating new experiences
into long-term memories goes wrong, it could result in the incorrect
association of a real memory with a mentally created experience, thereby
leading to delusions, he said. Tsien's study, published in the Nov. 10 issue of Science, also is interesting
in its development of a cutting-edge genetic engineering technique that allowed
him to control the function of a gene not only in a very specific region of the
brain, but also at specific points in time. He created a strain of mice that
had a modified version of a gene critical for memory formation. He constructed
this gene so that it would stop functioning when the animals received a dose of
the common antibiotic doxycycline in their drinking water. Taking the drug away
restored the gene to its normal function. The study focuses on a feature called the NMDA receptor, which studs the
surface of brain cells and which Tsien and others have shown to be critical for
the initial formation of memories. The NMDA receptor has been called a
"coincidence detector" because it receives signals from neighboring cells, but
only triggers a reaction when it receives two closely timed signals. This
characteristic allows the brain to associate two sensory inputs, such as a
voice and a face. In earlier studies, Tsien impaired learning and memory in mice by removing the
NMDA receptor, and enhanced those abilities by augmenting the receptor. (The
NMDA-enhanced mice have often been referred to as "smart mice.") In the new study, the researchers compared learning and memory in normal mice
and in those engineered to have an NMDA receptor that would turn off in a
specific region of the brain with a dose of doxycycline. In one test, the mice
were taught to find their way out of a tray of water by finding a hidden
platform. During seven training sessions, the mice all learned at the same
rate. They were then treated with doxycycline for a week and plain water for
another week. Retesting showed that the genetically modified mice that had
received the drug were significantly slower at finding their way out of the
water, even though they had initially been equally adept at it. Experiments
testing emotional memory showed similar results. The scientists also conducted tests in which they waited longer - until after
long-term memory was established - to administer the doxycycline. Those tests
showed no impairment of the ability to retrieve information, indicating that
NMDA receptor function in the hippocampus, a tiny region inside the brain, is
important for what scientists call "memory consolidation," but not retrieval. Current theory suggests that the shift from short- to long-term memory is
driven by a cascade of biochemical reactions unleashed by the original act of
learning. These reactions, including the creation of new proteins, build
connections between neurons, thus creating new permanent memories. That theory seemed flawed, said Tsien, because the cascade of reactions lasts
only a few hours or couple of days, and the consolidation of long-term memory
in the mammalian brain can take weeks, months or even years. "The time scale
simply doesn't match." The answer may be that something very similar to the
initial learning event happens again and again, a process Tsien calls synaptic
reentry reinforcement, or SRR. He believes SRR could be a model for
understanding memory over longer time scales. "Scientists are always mystified by how brain stays connected, how information
is stable for most of our lives," said Tsien. "This SRR process could be a
crucial mechanism to ensure the stored information is continually consolidated
and remains largely stable, despite of the constant turnover of the nuts and
bolts of our brains."
http://www.eurekalert.org/releases/pu-irs110900.html
 

 

(from Kabai P賥r: )