Stem Cell Therapy the Huard Way
by Dan Stimson
Twelve years ago, MDA-funded scientists began an ambitious clinical trial in
boys with Duchenne muscular dystrophy (DMD). In a procedure called myoblast
transfer, they removed immature muscle cells (myoblasts) from close male
relatives who didn't have DMD, and transplanted them directly into the boys'
muscles. The myoblasts were supposed to regenerate the boys' damaged muscles,
but they had little, if any, effect.
For cell biologist Johnny Huard (pronounced HEW-ard), who contributed to the
preclinical research on myoblast transfer and helped to conduct an arm of the
trial at Laval University in Quebec, the trial's failure left a lasting
impression.
"We had 11 patients coming to the hospital regularly and I became good friends
with them," Huard remembers. "For some of them, we increased their strength
temporarily, but the treatment didn't hold and we weren't able to save their
lives. I became very touched by those people."
Huard remained committed to finding a cure for DMD, but for a few years, he
shifted his research away from cell transplantation.
Then, research in the late 1990s set the stage for a new look at cell
transplantation for DMD and a host of other diseases. Scientists made several
breakthrough discoveries about embryonic stem cells — cells that aren't just
immature, but are nearly blank slates, capable of mass-producing the diverse
cell types that make up the human body (see "Embryonic Stem
Cells"). They came up with ways to grow stem cells in the laboratory,
and found a collection of stem cell "markers" — proteins that could be used to
identify stem cells and separate them from other cells.
Using those markers, Huard and other scientists began to fish for stem cells in
adult tissues — including bone marrow, brain and muscle. By combining the
markers with a new twist to his old myoblast isolation procedure, Huard
recently hit pay dirt — a type of stem cell derived from adult muscle that
appears to have an unmatched capacity for generating muscle. Armed with these
new cells, he's gearing up for another try at cell transplantation for DMD.
Stem Cells With Muscle
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| Johnny Huard demonstrates the procedure he developed for isolating
muscle-derived stem cells, which he hopes to use as a treatment for muscular
dystrophies. |
Myoblasts seemed to be effective at regenerating muscle tissue in mice with DMD,
so scientists were baffled when the cells fizzled in humans.
Some scientists returned to animal studies in hopes of improving myoblast
transfer and retesting it in people. Others spent years poring over tissue
samples from the dozens of boys who had undergone the procedure. They found
that some myoblasts were destroyed by the recipient's immune system, some
appeared to become dormant, and others failed to make dystrophin — the protein
that's missing in DMD.
Around that time, Huard was studying gene therapy for DMD, but in the dismal
results of myoblast transfer, he saw a glimmer of hope. Although the myoblasts
were duds overall, at least a small fraction of them, or perhaps some unknown
cells inadvertently mixed in with them, appeared to have myogenic potential
— the power to survive and produce muscle.
In hopes of finding those cells, he began to toy with his procedure for
isolating myoblasts from mice — which involves taking a sample of skeletal
(voluntary) muscle, and distilling it into a mixture of fluid and individual
cells suspended in a flask. After about a day, some of the cells begin to
attach to the flask — those are myoblasts.
"For years, we used to assume that if the cells didn't stick to the flask, they
were dead, so we threw them away," Huard says.
But when he waited a week for the floating cells to stick, he found what he'd
been looking for — cells with improved myogenic potential. And "when we started
testing them for stem cell markers, we found out they were stem cells," he
says.
| Stem Cell Jump-Start |
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In 1999, MDA grantees Louis Kunkel and Emanuela Gussoni of Children's Hospital in Boston isolated stem
cells from mouse muscle by revamping a procedure that had been used to isolate
stem cells from bone marrow. Then, they used a bone marrow transplant procedure
to deliver the cells to mice with DMD.
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| Mark Keating believes the regenerative powers of newts might hold clues to
repairing muscles destroyed by muscular dystrophy. |
The transplanted cells formed bone marrow in the mice, and a small fraction migrated away from the bone
marrow to form new muscle fibers — but not enough to have a therapeutic effect
(see "Renewing Muscles and Nerves," Quest, vol. 7, no. 2).
"The procedure just had very low efficiency, and it needs to be improved," Kunkel says. Damaged muscles
probably send out a distress signal that beckons stem cells from the bone
marrow, but the signal is weak, Kunkel believes. Finding a way to boost that
signal could be the key to making bone marrow transplants an effective
treatment for DMD and other types of muscle damage, he says.
In fact, many scientists have speculated that if there were a way to mobilize the stem cells in bone
marrow — or in other adult tissues — it might be possible to perform stem cell
therapy without a stem cell transplant.
Late last year, scientists reported they'd
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used that strategy to improve survival in mice following heart attack. Piero Anversa of New York Medical
College in Valhalla and his team injected the mice with two signaling proteins
called cytokines, then gave the mice heart attacks by
tying off blood vessels to their hearts. The cytokines coaxed stem cells
in the bone marrow to migrate through the bloodstream and repair the
damaged cardiac muscle.
The cues that attract stem cells from bone marrow to skeletal muscle are poorly understood, but research
by Mark Keating, also of Children's Hospital in Boston, suggests that one day
it might be possible to mobilize stem cells within muscle to regenerate lost
muscle fibers.
Keating studies regeneration in amphibians (frogs, newts and the like), which are known for their
remarkable ability to grow back an entire amputated limb — muscles, nerves and
all. "We don't think there's any reason mammals can't regenerate those things.
The difference is in the molecular cues, and we're trying to discover those,"
Keating says.
Amphibians owe much of their regenerative powers to a process called dedifferentiation, in which
a cell regresses from a specific (differentiated) cell type such as a muscle
cell or nerve cell to a type more like a stem cell.
A little over a year ago, Keating showed that a gene called msx1 can promote dedifferentiation in mouse
muscle cells. The gene is normally turned off in mature muscle cells, but when
Keating turned it on, the cells split apart and began to divide. And last
November, he reported that a liquid extract derived from newt limb had a
similar effect.
"This line of work has great promise for people with muscular dystrophy," Keating says. But he adds,
"[it's] all being done in animals, so it's still far away from anything that's
going to help patients."
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Stem Cell Transplants
Huard, who's now at Children's Hospital of Pittsburgh, isn't the first scientist
to isolate muscle-derived stem cells from mice (see "Stem Cell
Jump-Start"). But, in his effort to reinvent myoblast transfer, he's
the first to transplant muscle-derived stem cells directly into mouse muscle.
With support from MDA, he hopes eventually to bring the procedure to clinical
trials for DMD and other muscle diseases.
Muscle-derived stem cells, Huard believes, will succeed where myoblasts failed
because stem cells occur a step or two before myoblasts in the chain of command
for making new muscle.
Myoblasts form muscle; but the stem cells in muscle — perhaps reserved there
from embryonic life — form myoblasts. To produce new muscle tissue, a myoblast
fuses to an existing muscle fiber and thus ends its own short life. To produce
a myoblast, a stem cell splits in two, making a new cell and preserving itself.
This means that stem cells can make new muscle and keep making it long after
transplantation. It also means that muscle-derived stem cells lack most of the
characteristics of mature muscle, including cell surface proteins that can
trigger the immune system, leading to rejection of the transplanted cells. And
finally, there's evidence that the stem cells in muscle don't just produce
muscle fibers, but other cell types that might improve muscle regeneration.
One kind of stem cell transplant Huard is investigating — called an allogeneic transplant — is to use muscle-derived stem cells from healthy donors, the same
way myoblast transfer was done. "In the best-case scenario," he says, "we could
isolate cells from a single donor, grow millions of them in the lab, and then
inject 50 different patients."
But there's a drawback to that approach: Even though stem cells are believed to
possess few immune system triggers, many scientists fear that allogeneic stem
cell transplants might provoke the same type of immune rejection observed in
myoblast transfer.
| Embryonic Stem Cells: The Key to Treating Some Diseases? |
|
While research on adult-derived stem cells moves quietly forward, the debate over human embryonic stem
cells continues to resonate at full volume, frequently at the top of the news.
For most people, the debate is less about the stem cells — removed from the embryo when it's no bigger
than the tip of a pin — than about the embryo itself, which is destroyed in the
process.
Most people agree that human embryonic stem cells — the construction crew that assembles the human body
— hold the potential to replace cells lost to injuries and diseases, including
neuromuscular disorders. But opponents of research on the cells believe the
tiny embryo is a sacred human life. Supporters argue that the embryo is just a
clump of cells on its way to becoming human.
Among scientists, the debate has centered more on the cells themselves. Embryonic stem cells are capable
of making every cell type in the body, while adult-derived stem cells (though
they've proved surprisingly versatile) appear more restricted in their choices.
Some scientists believe that difference could make embryonic stem cells an
ideal therapeutic tool but others — like Johnny Huard — disagree.
"I don't see an advantage for me to work on human
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embryonic stem cells," says Huard of his
efforts to develop a stem cell treatment for muscular dystrophy.
"Embryonic stem cells can make anything, but they can also become tumors.
The cells we extract from adult muscle [in mice] are imprinted
[programmed] to make muscle."
Still, other scientists insist that human embryonic stem cells may hold advantages for treating some
diseases, in part because they're easy to manipulate into becoming certain cell
types, and because they're relatively easy to grow in the lab. The bottom line,
they say, is that the full therapeutic potential of embryonic stem cells will
never be known without further study.
In response to those concerns, President Bush announced last summer that he was lifting a moratorium on
federal funding for research on human embryonic stem cells. Under the new
policy, the government won't fund the destruction of human embryos, but will
fund research on 72 existing stem cell "lines" — colonies of laboratory-grown
cells derived from human embryos prior to Aug. 9, 2001.
On the advice of its research advisory committees, composed of leading scientists and physicians across
the country, MDA adheres to the same policy.
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So, Huard is looking into another possibility called an autologous transplant,
in which the goal is to isolate stem cells from someone with the disease and
transplant them into the same person. For someone with DMD or any other genetic
disease, the stem cells could be fixed with a corrective gene before they're
transplanted.
Promising Results
In December, at the annual meeting of the American Society for Cell Biology in
Washington, Huard reported that he'd tested both kinds of transplant in mice.
The results of those MDA-funded studies haven't yet been published, but are
being reviewed by the Journal of Cell Biology.
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| Huard and his colleagues discuss the differences between muscle-derived
stem cells and myoblasts — which could mean the difference between successful
therapy and failure. |
To test the autologous transplant approach, Huard and his colleagues isolated
stem cells from the muscles of mice with DMD, grew the cells in large numbers,
fixed them with a corrective dystrophin gene and reintroduced them into the
diseased mice. The stem cells made dystrophin-positive muscle fibers, though
not enough to restore normal muscle function.
The allogeneic transplants — injecting healthy donor-derived stem cells into the
muscles of mice with DMD — worked better, in some cases restoring dystrophin to
more than 25 percent of the cells in the injected muscle. That's probably
enough to improve the muscle's function, Huard says, noting that many boys with
Becker muscular dystrophy, a less severe version of DMD, have a similar
fraction of dystrophin-positive fibers. "We're doing the strength analysis [on
the mice] right now," he says.
Another interesting result of the allogeneic transplant is that "[the injected]
stem cells didn't just make muscle fibers. They made blood vessels, and they
made peripheral nerve," Huard said. For boys with DMD, this could turn out to
be beneficial, especially in older boys who might have secondary damage to the
vasculature and nerves connected to their muscles.
How Stem Cells Might Be Used
to Treat Muscular Dystrophy |
| ALLOGENEIC TRANSPLANT |
| (1) A sample of muscle is removed from a healthy donor |
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| (2) Stem cells are isolated and grown in the lab |
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| (3) Stem cells are injected into muscles of the person with the disease |
|
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| AUTOLOGOUS TRANSPLANT |
| (1) A sample of muscle is removed from the person with the disease |
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| (2) Stem cells are isolated and grown in the lab |
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| (3) The stem cells are treated with a virus that carries the corrective gene |
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| (4) The treated stem cells are injected back into the person's muscles |
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Next, Huard plans to test stem cell transplants in animals larger than mice,
determine whether the cells carry any risk of forming tumors and, perhaps most
importantly, find cells from human muscle tissue that are equivalent to the
mouse stem cells he's been studying.
Without those crucial experiments, "stem cells aren't yet ready for clinical
trials," he says. But he has consulted with the Food and Drug Administration in
preparation for a trial in youngsters with DMD.
Eventually, Huard hopes to use a combination of muscle stem cell transplants to
strengthen voluntary muscle and intravenous systemic delivery of stem cells to
restore dystrophin in the heart and diaphragm. 
Editor's note: A few private companies currently offer variations of myoblast
transfer or stem cell therapy for DMD. These procedures, in which one "shot" of
cells can carry a price tag of $100,000 or more, aren't approved by the FDA
(hence, they're only available overseas). It's MDA's position that the
treatments haven't been adequately tested for safety or effectiveness. |
