MDA Gathers Scientists, Physicians
for Updates on Research Progress
Some 220 professionals — physicians associated with MDA
who treat patients with neuromuscular diseases, and MDA-supported
scientists conducting research in these conditions — gathered
in Tucson, Ariz., Nov. 17 through Nov. 19 for Translating Basic
Research Into Clinical Strategies.
MDA and the University of Arizona College of Medicine sponsored
the conference, which was chaired by neurologist Jerry Mendell
of Ohio State University and Columbus (Ohio) Children’s
Research Institute, and biochemist Kevin Campbell at the University
of Iowa, both longtime MDA grantees.
Duchenne MD: Gene Rereading, Gene Transfer
Among the conference’s highlights were several demonstrations
of how careful study of the gene for dystrophin, the protein
missing in boys with Duchenne muscular dystrophy (DMD), has
resulted in strategies for treating the disease.
Steven Wilton, an MDA grantee at the University of Western
Australia in Perth, described a technique called exon skipping for the treatment of DMD. Wilton’s strategy, made possible
by years of MDA-supported study of the gene for dystrophin,
takes advantage of the way dystrophin DNA, after being converted
to RNA, is processed, prior to synthesis of the dystrophin protein.
Exons, the parts of an RNA strand that are reflected in the
final structure of the protein, are interrupted by introns,
which are removed from the RNA by the cell’s processing
mechanisms. Wilton and colleagues have developed a method for
coaxing cells to ignore exons containing genetic errors (mutations)
and splicing together exons on either side of them, thereby
allowing a nearly normal dystrophin protein to be made.
MDA grantee H. Lee Sweeney, from the University of Pennsylvania,
described another molecular strategy for the treatment of DMD,
which is further along in the drug development pipeline. In
this approach, called stop codon read-through, cells
are encouraged to ignore erroneous (premature) stop signals
in the dystrophin gene thought to cause DMD in approximately
15 percent of boys with the disease. These premature stop signals
cause a shortened and nonfunctional protein to be made.
PTC Therapeutics, a biotech company in South Plainfield, N.J.,
with support from MDA and basic science contributions from Sweeney,
has developed an experimental drug called PTC124 that’s
slated for testing in boys with DMD this year. It has already
been tested and found safe in healthy volunteers.
Identification of boys with premature stop signals in the dystrophin
gene has been made possible by meticulous study of the gene
and development of new methods for pinpointing each patient’s
precise mutation. Flanigan described his laboratory’s
method for such precise diagnosis by complete sequencing of
the dystrophin gene.
University of Washington-Seattle biologist Jeffrey Chamberlain,
a longtime MDA grantee, showed how mice missing both dystrophin
and a closely related compound, utrophin, and therefore showing
severe MD symptoms, were helped by a single injection of highly
miniaturized dystrophin genes into the bloodstream at 1 month
of age.
Chamberlain’s group learned how to make the miniaturized
(microdystrophin) genes after years of study to determine which
parts of the very large dystrophin gene were essential and which
could be eliminated. The microdystrophin genes they created
fit into a highly effective and apparently safe adeno-associated
virus (AAV) delivery vehicle. These mice were injected with
microdystrophin genes inside type 6 AAV shells.
(For more on gene rereading strategies, see “Changing
the Code.” For an overview of gene transfer, see “Bridge
Over Troubled Waters.”
Mitochondrial Disease: Targeting Miniorgans
Eric Schon, a molecular biologist at Columbia University in
New York, thanked MDA for support over the years to his study
of mitochondria, the miniature organs inside cells that produce
most of the cells’ energy. When things go wrong in these
miniorgans (organelles), as happens in the mitochondrial myopathies,
adverse effects on the muscles and nervous system can be severe.
Schon explained that mitochondria have their own DNA but also
rely on DNA from the cell nucleus to carry out their functions.
In Schon’s laboratory, potentially therapeutic DNA can
be inserted into a cell nucleus with a tag that tells the cell
to send the newly made protein to the mitochondria. His lab
group has also attacked mutations in mitochondrial DNA by inserting
a highly targeted DNA-cutting enzyme that snips out a mitochondrial
DNA mutation and leaves intact the surrounding, normal DNA.
Myasthenias: Refining Signals
Disorders of nerve-to-muscle signal transmission, known as myasthenias, can be either acquired or genetic. Donald
Sanders, who co-directs the MDA clinic at Duke University Medical
Center, described how basic science research that increased
understanding of MuSK, a protein on the muscle side of the nerve-to-muscle
(neuromuscular) junction, led physicians to recognize a new
type of myasthenia gravis (MG),
in which the immune system attacks this protein.
In the more common type of MG, the immune system attacks the
acetylcholine receptors, “landing pads” on muscle
cells where nerve signals are received.
C. Michel Harper, who works with longtime MDA grantee Andrew
Engel at the Mayo Clinic in Rochester, Minn., described how
basic research on the neuromuscular junction has resulted in
the understanding of how genetic mutations affect the way acetylcholine,
a signal-transmitting chemical, is packaged, transmitted, received
or broken down.
Defects in these processes can lead to distinct congenital
myasthenic syndromes, each of which requires a treatment tailored
to the underlying molecular defect. |
