Neuroscientists have isolated the “when” and “where” of molecular
activity that occurs in the formation of short-, intermediate-, and
long-term memories
Neuroscientists from New York University and the University of
California, Irvine have isolated the "when" and "where" of molecular
activity that occurs in the formation of short-, intermediate-, and
long-term memories. Their findings, which appear in the journal the Proceedings of the National Academy of Sciences,
offer new insights into the molecular architecture of memory formation
and, with it, a better roadmap for developing therapeutic interventions
for related afflictions.
"Our findings provide a deeper understanding of how memories are
created," explained the research team leader Thomas Carew, a professor
in NYU's Center for Neural Science and dean of NYU's Faculty of Arts and
Science. "Memory formation is not simply a matter of turning molecules
on and off; rather, it results from a complex temporal and spatial
relationship of molecular interaction and movement."
Neuroscientists have previously uncovered different aspects of
molecular signaling relevant to the formation of memories. But less
understood is the spatial relationship between molecules and when they
are active during this process.
To address this question, the researchers studied the neurons in
Aplysia californica, the California sea slug. Aplysia is a model
organism that is quite powerful for this type of research because its
neurons are 10 to 50 times larger than those of higher organisms, such
as vertebrates, and it possesses a relatively small network of neurons
-- characteristics that readily allow for the examination of molecular
signaling during memory formation. Moreover, its coding mechanism for
memories is highly conserved in evolution, and thus is similar to that
of mammals, making it an appropriate model for understanding how this
process works in humans.
The scientists focused their study on two molecules, MAPK and PKA,
which earlier research has shown to be involved in many forms of memory
and synaptic plasticity -- that is, changes in the brain that occur
after neuronal interaction. But less understood was how and where these
molecules interacted.
To explore this, the researchers subjected the sea slugs to
sensitization training, which induces increased behavioral reflex
responsiveness following mild tail shock, or in this study, mild
activation of the nerve form the tail. They then examined the subsequent
molecular activity of both MAPK and PKA. Both molecules have been shown
to be involved in the formation of memory for sensitization, but the
nature of their interaction is less clear.
What they found was MAPK and PKA coordinate their activity both
spatially and temporally in the formation of memories. Specifically, in
the formation of intermediate-term (i.e., hours) and long-term (i.e.,
days) memories, both MAPK and PKA activity occur, with MAPK spurring PKA
action. By contrast, for short-term memories (i.e., less than 30
minutes), only PKA is active, with no involvement of MAPK.
The study's other co-authors were Xiaojing Ye, a postdoctoral fellow
in NYU's Center for Neural Science, Andreea Marina, an undergraduate at
UC Irvine at the time of the study. The research was conducted at NYU's
Center for Neural Science and UC Irvine's Center for Neurobiology of
Learning and Memory.
This work was supported by grants RO1 MH 041083 and RO1 MH 081151
from the National Institute of Mental Health, part of the National
Institutes of Health, and a grant IOB-0444762 from the National Science
Foundation.
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