THURSDAY, June 5 (HealthDay News) -- Researchers report they
have used neural stem cells to correct a congenital brain disorder
in mice.
Dr. Steven Goldman, of the University of Rochester Medical
Center in New York, and his colleagues used a type of neural stem
cell called "glial progenitor cells" (GPCs), derived from human
fetuses, to correct both behavioral and physiological abnormalities
in a mouse model of a myelin-deficiency disorder.
The study represents "a very important advance," said Dr. James
Goldman, an investigator in the Columbia Neural Stem Cell Program
at Columbia University Medical Center, who was not involved in the
study.
Though Steven Goldman and others previously had shown that
injection of GPCs into mouse brains could lead to remyelination of
demyelinated neurons, that observation did not include any change
in disease progression.
"The fact that they were able to get at least some of these
animals to survive, and show that physiologically and behaviorally
they are doing well, is an advance," said James Goldman.
The findings were reported in the June issue of
Cell Stem Cell.
Myelin is a structure, comprised of protein and fat, that
envelops long neuronal fibers called axons. Axons are the conduits
for neural impulses, both conscious and unconscious. Just as
electrical cable must be insulated to prevent signal loss over
distance, myelin ensures that nerve impulses can traverse long
axonal processes in the central nervous system without
degrading.
Myelin is formed by neural support cells called
oligodendrocytes, which are derived from GPCs. Disorders that arise
from the absence or degradation of myelin represent a "substantial
proportion of adult neurological diseases," said Steven Goldman.
They run the gamut, from autoimmune disorders like muscular
dystrophy, to lysosomal storage diseases like Tay-Sachs, to
congenital defects like Pelizaeus-Merzbacher Disease, an X-linked
condition where myelin doesn't form.
In this study, Goldman and his team used "shiverer" mice, whose
congenital lack of myelin basic protein causes them to shake and
seize uncontrollably, giving them their name. They typically die by
5 months of age.
The shiverer mice were crossed with immunodeficient mice, so
they would not reject the GPC transplant, and split into three
treatment groups; 59 received no treatment, 29 received injections
of buffer into five different locations in the brain shortly after
birth, and 26 received injections of GPCs.
By about 130 days after birth, all 88 control mice died. But six
of 26 transplanted animals survived at least 160 days, and four
lived over a year. Behaviorally and physiologically, these
survivors appeared largely cured, and post-mortem analysis of these
animals' brains and spinal cords demonstrated why.
"The entire central nervous system had remyelinated and looked
normal in terms of structural configuration of the myelination,
both at the microscopic and submicroscopic level, and at the
behavioral level," Goldman said.
In other words, from five separate injection sites, the GPCs
migrated throughout the central nervous system, differentiated into
oligodendrocytes, and began producing myelin.
The researchers then assessed the physiological effect of that
remyelination, by measuring the speed of nerve transmission along
remyelinated axons. They observed velocities on par with those of
normal mice.
"That is proof in principle that putting glial progenitors in a
brain like this will at least partially remyelinate the brain, and
do so functionally," said James Goldman.
Though this study involved a congenital pediatric disorder,
Steven Goldman said his goal is to apply the technique to adult
diseases like multiple sclerosis. For now, his team is working to
understand why most transplanted animals still die. He suggested
this could stem from the seizures that plague shiverer animals,
including transplant recipients that have not yet completed
remyelination, and said he is exploring the utility of pairing
transplants with anticonvulsant therapy to alleviate this
problem.
But James Goldman pointed out that before this transplant
procedure can be turned into a clinical therapy, several issues
must be addressed, not the least of which is the politically
sensitive problem of obtaining and using human fetal tissue as a
therapeutic agent.
More information
For more on leukodystrophies, visit the
U.S. National Library of Medicine.
