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September 8, 1999
Media contact:
Leslie Franz, UCSD, (619)
543-6163
For
Salk:
Suzanne Clancy (858) 453-4100 ext. 1340
Warren Froelich (858)
453-4100 ext. 1646
AGE-ASSOCIATED
MEMORY LOSS MIGHT BE REVERSIBLE
Researchers from the University of California, San
Diego and the Salk Institute for Biological Studies have identified a
process by which the normal primate brain degenerates with aging, and
have also shown that this degeneration can be reversed by gene
therapy.
While
normal aging often results in some loss of memory and other cognitive
functions, scientists have been unable to pinpoint changes in specific
anatomical regions of the brain associated with these processes which
might explain this decline.
New research published in the
September 14 issue of the Proceedings of the National Academy of
Science (PNAS) suggests that the age-related breakdown is occurring in
the cells of the system that activates brain function in the
hippocampus and cortex, which are the primary sites of memory,
selective attention and other cognitive functions.
The good news is that in primates,
the degeneration that occurs in this system appears to be almost
completely reversible when tissue grafts of genetically modified cells
that deliver human nerve growth factor (NGF) to the impaired cells are
implanted in the brain.
The PNAS study was conducted in
rhesus monkeys, which provide a good model for human aging. The target
of the study was the subcortical system, a signaling system of
cholinergic neurons that regulate cortical and hippocampal activity.
The monkeys were housed at the California Regional Primate
Research Center at the University of California, Davis.
“Our findings show that with
normal aging, there is a significant loss of function and shrinkage in
size of neurons in a subcortical system called the ‘cholinergic
system’,” said the senior author of the PNAS paper Mark Tuszynski,
M.D., Ph.D., associate professor of neurosciences at the University of
California, San Diego School of Medicine and neurologist with the
Veterans Affairs San Diego Health Care System. “These cholinergic
neurons, through the release of neurotransmitters, basically regulate
the voltage and activity of cells in the cortex and hippocampus,
allowing the cortex to process information and function normally.
They essentially ‘prime’ the
brain to function, so, if as a result of normal aging their activity
is turned down, the brain’s ability to process information is
hampered.
“Equally
important is the evidence that these neurons are not dead, just
atrophied with aging.
They can be returned to what appears to be a normal state with
a gene therapy approach that delivers NGF to the cells,” he said.
According to Tuszynski, these
findings have implications not only for cognitive function in normal
aging, but might also be significant in preventing some of the
cognitive decline in neurodegenerative conditions such as
Alzheimer’s disease, in which this same system of cells is known to
undergo profound atrophy and death.
Four groups of monkeys were
studied.
One group of young monkeys and a group of normal aged monkeys
were compared in order to identify the changes in neurons associated
with age.
In addition, a group of aged monkeys which received brain
grafts of genetically modified NGF-secreting tissue, and a control
group of aged monkeys which received non-NGF grafts, were studied to
see whether NGF tissue grafts would have any effect.
NGF is essential for the normal development of these neurons in
the fetus, and the brain remains sensitive to NGF throughout life.
In the normal aged monkeys, the
number of subcortical cholinergic neurons making proper amounts of
neurotransmitters and receptors for growth factors declined by 43
percent compared with the young monkeys, and the remaining neurons
were 10 percent smaller.
The aged control monkeys with non-NGF-secreting tissue implants
showed identical losses.
However,
aged monkeys which received NGF-secreting grafts showed an almost
complete restoration of normal cell function in 92 percent of neurons,
and size returned to within 3 percent of normal.
“Normal
aging affects not only memory, but perhaps more importantly things
like attention, the ability to focus on multiple tasks at once, and
the overall efficiency of thought processes,” said Tuszynski.
“In the case of conditions like Alzheimer’s disease, which affects
approximately 4 million people, this decline in function is even more
severe. These findings give
us a new avenue to pursue in trying to enhance these functions in both
the normal aged brain and in the diseased brain.”
This study looked strictly at the
measurable physical indications of atrophy and regeneration.
Tuszynski said studies also are being done to evaluate
behavioral and functional changes.
Co-authors of the PNAS paper are
David Smith, M.S., a graduate student at the UCSD School of Medicine;
Jeff Roberts, D.V.M., of the California Regional Primate Research
Center at UC Davis; and Fred H. Gage, Ph.D., of the Salk Institute for
Biological Studies.
This
work was supported by grants from the National Institutes of Health,
the Department of Veterans Affairs, and the California Regional
Primate Research Center. |
