Published: February 03, 2011
UM Researchers Identify New Gene Causing Blindness
MIAMI - (BUSINESS WIRE) - Researchers led by geneticists at the University
of Miami Miller School of Medicine have identified a new gene that
causes retinitis pigmentosa, a form of blindness, ending one South
Florida family's nearly 20-year search for what caused three of their
four children to lose their sight.
The Lidsky children, who are now in their 30s, began to lose their sight
in their teens. Their parents, Betti and Carlos, had the family's DNA
tested for more than 50 retinitis pigmentosa (RP) genes. No one found
the link until they began working with UM researchers in late 2009. By
the summer of 2010, researchers had found the cause of their retinitis
pigmentosa using exome sequencing and confirmed it with zebrafish
studies.
"For 18 years, we have been searching for the genetic cause of this
disease and UM researchers have found it," Mrs. Lidsky said. "We've
wanted this for some time. These researchers are truly our heroes. They
are doing life-changing work that will benefit not only our family but
many other people. We are truly grateful for all their hard work."
The result of the work, a paper titled "Whole-exome sequencing links a
variant in DHDDS to retinitis pigmentosa," was published online
Thursday, February 3, in the American Journal of Human Genetics.
To identify the gene responsible for retinitis pigmentosa in the Lidsky
family, researchers used a new technology known as whole exome
sequencing, which thoroughly investigates the coding portions of an
individual's genetic material. The RP gene identified in this family
codes for an enzyme known as dehydrodolichol diphosphate synthase
or DHDDS, which is thought to play a role in how a light-sensing
protein named rhodopsin works.
The research was led by Margaret A. Pericak-Vance, Ph.D., associate dean
for human genomic programs, the Dr. John T. Macdonald Foundation
Professor of Human Genomics, and director of the John
P. Hussman Institute for Human Genomics, along with Stephan Zuchner,
M.D., Ph.D., first author of the paper and director of the Center for
Human Molecular Genomics at the Hussman Institute, and Byron Lam, M.D.,
professor of ophthalmology at Bascom
Palmer Eye Institute.
"This was a powerful demonstration of what we can do with new genetic
technologies," Dr. Zuchner said. Important evidence to support this gene
as the cause of RP comes from research with zebrafish, led by
collaborator Julia Dallman, Ph.D., in the Department
of Biology at UM. When researchers in her lab blocked the enzyme,
the fish became blind.
Researchers from five areas of the University of Miami -- the John P.
Hussman Institute for Human Genomics, the Dr. John T. Macdonald
Foundation Department of Human Genetics, Bascom Palmer Eye Institute,
the Department
of Biochemistry and Molecular Biology, and the Department of Biology
- worked together to make this exciting discovery. Researchers from the
Department of Psychiatry at Mount Sinai School of Medicine and the
Center for Human Genetics Research at Vanderbilt University School of
Medicine also contributed to the work.
"This research brings hope to families that have rare genetic diseases
whose causes had formerly eluded researchers using traditional methods,"
said Dr. Pericak-Vance, senior author on the paper. "We now can bring
hope to families who formerly thought their situation was hopeless."
"This is another example of how genomics research is critically
important to our work here at the Miller School of Medicine," said
Pascal J. Goldschmidt, M.D., Senior Vice President for Medical Affairs
and Dean of the Miller School. "It makes a difference in people's lives.
In addition, it exemplifies the team approach to research we take here
at UM."
Retinitis pigmentosa refers to a large group of diseases that cause
degeneration of the retina of the eye. The retina is located at the back
of the eye and its role is to capture light that enters the eye, which
is translated into images by the brain. In RP there is damage to the
cells in the retina that capture light, known as cones and rods. Over
time, these cells slowly stop working and vision deteriorates. One of
the first signs of RP is night-blindness, or the slow adaptation to dim
light. As RP progresses, people develop tunnel vision, which can
eventually lead to a complete loss of vision. RP is diagnosed in
approximately 1 in 3,000 to 4,500 people and is known to be caused by
changes, or mutations, in many genes.
Dr. Lam has treated the Lidsky siblings with retinitis pigmentosa -
Isaac Lidsky, Daria Zawadzki, and Ilana McGuinn - for several years. He
called the RP finding an "exciting discovery."
"Our success in identifying this novel DHDDS gene associated with
retinitis pigmentosa demonstrates the power of new genetic methodology
to find the cause of disease in small families," said Dr. Lam. "Finding
the genetic causes of retinal degeneration is important because it will
lead to a better understanding of retinal biology overall."
"The current findings will encourage further studies designed to examine
the role of proteins in the formation and renewal of light-sensitive
photoreceptor cells in the retina and how retinitis pigmentosa occurs,"
said Eduardo Alfonso, M.D., chair of Bascom Palmer Eye Institute. "The
ultimate implications are better patient care and the possibility of
developing new therapies."
While there is no cure for RP at this time, HIHG and Bascom Palmer
researchers said the discovery holds promise to develop new avenues for
therapy.
"We need to come at this from different angles," explained Jeffery M.
Vance, M.D., Ph.D., professor and chair of the Dr.
John T. Macdonald Foundation Department of Human Genetics, professor
of neurology and director of the Center for Genomic Medicine at the
Hussman Institute for Human Genomics. Dr. Vance is also a co-author on
the paper. "UM researchers are creating models using both zebrafish and
skin cells from patients to develop possible treatments, but they will
take some time to test."

University of Miami Miller School of Medicine
Jeanne Krull,
305-243-4853
JKrull@med.miami.edu
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