Brain May Be Easier To Repair Than Previously Thought
By Ronald Kotulak, Chicago Tribune
After 10 years, the drugs Dr. Jacqueline Winterkorn had been taking to
quell the shaking and immobility of Parkinson's disease were wearing
off.
''It's a very sad disease,'' she said. ''People are locked into bodies
that don't move. Their brains are working, their minds are working, but
they can't talk and they can't move.''
That changed a year-and-a-half ago when Winterkorn was given millions
of new fetal brain cells to replace those that were supposed to be
producing dopamine to control her movements, but instead were dying
off.
The new cells took up residence in her brain, extending delicate
tendrils to motor neuron cells, supplying them once again with
dopamine.
This is not a cure, Winterkorn, who lives in Roxbury, Conn., is quick
to say. But she estimates the brain tissue transplant improved her
mobility by about 30 prcent.
Wintoneers, who arel transpants to repair n's disease, stroke,
Huntington's disease and epilepsy, are providing important new evidence
that the brain may be a lot easier to repair than previously thought.
''The prospect of repairing a damaged brain is pretty remarkable,''
said Dr. Curt Freed of the University of Colorado Health Sciences
Center in Denver, who headed the just-completed Parkinson's transplant
study.
''It has been possible to show significant improvements in some
patients who suffered from a chronic neurologic disease for an average
of 14 years.''
New research is overturning old notions about how the brain works. Once
thought to be unchangeable, unrepairable and constantly losing neurons,
the brain is now seen to be always changing, eminently repairable and
constantly making new cells.
One of the new findings, which has enormous implications, involves
brain stem cells, a newly discovered cell line that has the almost
magical ability to make every other type of brain cell, including more
of itself.
Preliminary experiments in animals suggest that it may be possible to
inject brain stem cells into patients with a wide range of mental
disorders to cure diseases ranging from Alzheimer's disease to multiple
sclerosis.
The first results in mice show that mouse brain stem cells find their
way to areas of the brain with damaged cells like millions of Tarzans
swinging through a jungle of trees, make healthy copies of the wrecked
cells and correct the disorder, in this case an animal model of
multiple sclerosis.
Scientists don't know how stem cells do this, but they believe that the
brain and the stem cells talk to each other using a chemical language.
In a sense, stem cells ask every cell they encounter ''Are you OK?'' If
not, they pop out a healthy cell to take over the job of the sick one.
''A few years ago people looked at the adult brain and saw it in a very
static way,'' said Dr. Ronald McKay, chief of molecular biology at the
National Institute of Neurological Disorders and Stroke.
''Now we know it's a very dynamic structure,'' he said. ''The way the
brain works is controlled by signals that are passed between cells. It
gives us much more hope that we can understand these signals and use
that understanding to control the diseases of the nervous system.''
If transplanted stem cells work as well in humans, then replacing
errant brain cells with normal ones raises the possibility of fixing an
entirely different class of mental disorders, from schizophrenia to
depression.
''This is a dramatic new way of looking at both the development and
repair of the brain,'' said Dr. Evan Snyder of Harvard Medical School
and Children's Hospital in Boston, who reported isolating human brain
stem cells from fetal tissue last November.
''There's a whole new class of brain diseases that can now be
approached that couldn't before,'' he said.
Another new finding indicates that the brain may be able to regenerate
itself like the liver.
Instead of losing copious amounts of brain cells with age, human brains
may be doing just the opposite, making thousands of new ones every day.
This possibility is based on research showing that adult rats
continually make new cells in the hippocampus, an area of the brain
important for learning and memory. In an earlier report, Fred Gage of
the University of California at San Diego found that adult humans also
make new hippocampal cells.
The trick to keeping these new cells is a type of learning that
requires making associations that are separated either in time or
space.
Rats given new tasks to learn make use of the newly made brain cells,
incorporating them as permanent structures in the brain. Rats that do
not experience lerning lose the cells.
''The fact that learning specifically rescues these new cels from
death s that they aren not just that ning,'' said neld of
Princeton University, who has so far found the overproduction of new
brain cells in rat and monkey hippocampuses.
The ability of the brain to make loads of new brain cells in the
hippocampus opens th door to brain elf-repair, especially if other
areas of the brain also generate fresh cells. The key is learning how
to turn up an individual's own stem cell production to replace
defective neurons.
''I think we can use this naturally occurring regeneration to devise
strategies for repairing damaged brain regions,'' Gould said.
Enhancing the brain's own recuperative powers could ease the
controversy over the use of human fetal brain cells, which are obtained
from aborted fetuses. The National Institutes of Health has lifted its
ban on the use of human fetal cells and is funding a number of studies
involving their use.
While human trials using stem cell transplants, or the brain's own
regenerative capacity, may still be years away, fetal transplants for
Parkinson's diseas and other neurroblems involving localized
damage appear to be on the horizon.
The partial success experienced by Winterkorn resulted from a
double-blind, placebo controlled study involving 40 patients. Half
received fetal cells and the other half went through the surgery and
skull-drilling, but did not receive new dopamine-producing cels.
''A doule-blind study is unusual in surgery, but it's the only way to
prove a treatment has an effect or not,'' Winterkorn said.
Freed, who headed the study, said that a third of the patients who
received fetal cells did extremely well, a third hd some benefit,
a third either stayed the same or got worse.
After the study was over and the results announced, almost all of the
patients who served as controls, who had the surgery but did not
receive fetal cells, opted to get the cells in a second round of
surgery.
Patients under the age of 60, who received fetal cells, did the best,
while those older than 60 showed less improvement. Nevertheless, PET
brain images showed that the transplanted cells grew in the brains of
both the younger and older patients.
''That's a very interesting finding, that even if you're 70 plus years
old a fetal dopamine cell transplant can survive, grow and develop in
your brain,'' Freed said.
The next step is to see if the overall graft survival rate can be
significantly increased, particularly in older patients, by bathing the
fetal cells in growth factors, he said. Animal experiments show that
such growth factors as FGF and IGF-1, which normally promote brain
health and development, increase the transplant success rate, he added.
''There's growing optimism that fetal tissue transplants for
Parkinson's disease will work,'' said Dr. Jeffrey Kordower, a
Rush-Presbyterian-St. Luke's medical center neurologist, who is
participating in a second ongoing transplant study for Parkinson's
patients.
Kordower's autopsy studies of brain tissue from two patients who had
received fetal cells, and who died from unrelated causes, showed that
the fetal cells had taken root.
''The cells made connections with the host,'' he explained. ''They did
great. And the patients had done well, they had improved.''
Similar results have been achieved in stroke patients. At the
University of Pittsburgh Medical Center, neurosurgeon Dr. Douglas
Kondziolka implanted adult neurons into the brains of 12 patients who
suffered strokes as long as 6 years ago.
Preliminary results indicate that 8 patients reported improvements in
such capacities as speech, memory and muscle control. These patients
suffered strokes in an area of the brain called the basal ganglia,
which serves as a switching center for incoming and outgoing messages.
''We think that the improvement is related to cells hooking up with
existing cells that did not die in the stroke and are now providing a
better infrastructure for brain function,'' Kondziolka said.
The implanted neurons, which are commercially available, are derived
from an unusual 25-year-old tumor that can be made to produce mature
human brain cells. Once they become mature, they no longer are
cancerous.
Transplants of fetal tissue and mature neurons may provide local brain
repairs, but stem cells offer the opportunity to perform total brain
repairs, such as for diseases like Alzheimer's where vast portions of
the brain are eaten away, McKay said.
''It's fair to say that stem cells represent a breakthrough because of
their remarkable properties,'' he said. ''Stem cells will move long
distances, and large numbers of them will incorporate into the brain.
It's as if the brain is not a solid barrier. Stem cells can move
through it.''
As they move through the brain, stem cells look for damaged or
inoperative cells and stop to make healthy copies. Snyder's studies
with shiverer mice -- so-called because they have a neurodegenerative
disorder that causes them to shiver and die young -- revealed that
injected stem cells locate the trouble, mutated oligodendrocytes, which
are supposed to make myelin to insulate neurons.
Without their protective myelin coat, brain cells are unable to
properly conduct electrical signals. The mice develop tremors, a
symptom characteristic of multiple sclerosis, a human demyelinating
disease.
Snyder isolated stem cells from a mouse 13 years ago without knowing
what they were at the time. Only after years of research showed that
these cells could make all the other cells in the brain, were they
declared to be stem cells.
Injected into the brains of shiverer mice, stem cells swung from cell
to cell, pausing at the dysfunctional oligodendrocytes to make good
copies.
''Stem cells are very opportunistic,'' Snyder said. ''They love to
migrate by themselves or on anything that has a surface.''
Stem cells did their job in the shiverer mice. Myelin production
started up. As insulation grew around neurons, shivering slowed and
often stopped. Sixty percent of the treated animals improved, and some of them appeare to be completely normal.
Injecting the newly discovered human stem cells into mice with a
genetic condition that resembles Tay-Sachs disease, Snyder and his
colleagues found that the human cells traveled to the affected area of
the brain and made neurons that pumped out the vital chemical missing
in the disease. Further studies must be carried out to determine if the
stem cell transplant helped the Tay-Sachs mice.
If all goes well, human trials with stem cells may begin within five
years, probably with Alzheimer's patients, Snyder said.
Stem cells can be grown in unlimited numbers from a single source, and
the hope is that they can be used to treat all types of mental
disorders without incurring rejection problems, he said.
''The neural stem cell is a powerful new addition that really opens up
whole new vistas,'' Snyder said. ''For now, the stem cells and brain
cells talk to each other to heal things and we don't even know what
that language is. But we intend to learn it.''
