STUDIES SUPPORT ROLE OF GLUTAMATE, RNA PROCESSING
IN LOU GEHRIG’S DISEASE
TUCSON, Ariz., March 5, 2004 — The
possibility that a central nervous system
signaling chemical called glutamate
has a role in the development or exacerbation
of amyotrophic
lateral sclerosis (ALS, or Lou Gehrig’s
disease) has been strengthened by two
recent studies, the Muscular Dystrophy
Association announced today.
The findings suggest targets for future
therapies in this paralyzing disease,
which generally strikes adults in late
middle age, and is usually fatal within
five years.
“We’re really excited about
these findings,” said Sharon Hesterlee,
MDA’s research development director.
“We’ve known about the involvement
of glutamate in ALS for some time now,
but here we have some new clues as to
how this chemical may go wrong.”
MDA research grantee Jeffrey Rothstein
of the Department of Neurology at Johns
Hopkins University School of Medicine
in Baltimore, where he also directs
an MDA-supported ALS Center, was part
of a research team that published findings
online in Annals of Neurology, showing
that people with ALS make a variant
form of a protein whose usual role is
to remove glutamate after it has carried
a signal from one nerve cell to another.
This type of protein is called a glutamate
transporter, and it’s vital for
keeping glutamate from building up and
poisoning cells.
The type of transporter made by the
ALS patients may not be as good as the
one normally produced, the researchers
suggest, although they haven’t
yet proven that.
They do know that the difference in
the two transport proteins — EAAT2
and EAAT2b — comes about because
of a change in the way RNA, the chemical
that’s made from DNA and immediately
precedes protein manufacturing, is assembled,
a process known as “RNA splicing.”
And they also know that glutamate transport
is known to be faulty in people with
ALS whose tissues have been studied
to detect this problem.
In a separate study, a Japanese research
group found that samples of muscle-controlling
nerve cells from ALS patients are different
from those of people without ALS in
another way — but one that also
implicates both glutamate and RNA processing.
Shin Kwak of the Department of Neurology
at the University of Tokyo found that
56 percent of the nerve cells examined
from people with ALS contained abnormal
glutamate receptors sites on the cell
surface where glutamate normally docks.
None of these abnormal receptors were
found in cells taken from people who
didn’t have ALS.
The kind of receptor that most people
have keeps calcium out of the targeted
cell, while the kind that was found
in the ALS patients allows calcium to
gain entry. Since excess calcium in
the wrong place is a well-known cause
of cell death, the calcium-permeable
glutamate receptors could be a key factor
in the disease.
The Japanese researchers, who published
in the journal Nature, say that the
nerve cells of ALS patients can’t
perform a vital step in the final stages
of RNA processing which makes the difference
between a receptor that lets calcium
through and one that doesn’t.
Rothstein, who has been studying glutamate
transport for about a decade, said the
Japanese finding describes “another
hit in the glutamate pathway.”
He says both findings help build the
argument for the key role of glutamate
signaling in ALS.
The only treatment approved by the U.S.
Food and Drug Administration for ALS
at this time is riluzole, a drug that
partially blocks glutamate in the nervous
system.
“You can manipulate the glutamate
system,” Rothstein says. But he
adds that researchers might now also
be able to target the RNA processing
errors uncovered by these two studies.
“There are RNA editing and splicing
enzymes,” he says, offering these
as possible areas for investigation.
“Anything that gives you new targets
is good.”
MDA is a voluntary health agency working
to defeat ALS and more than 40 other
neuromuscular diseases through programs
of worldwide research, comprehensive
services, and far-reaching professional
and public health education.
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