Gene mutation linked to retinitis pigmentosa in Southwestern U.S. Hispanic families
University of Texas Health Science Center at Houston News Jun 30, 2017
Thirty–six percent of Hispanic families in the U.S. with a common form of retinitis pigmentosa got the disease because they carry a mutation of the arrestin–1 gene, according to a new study from researchers at The University of Texas Health Science Center at Houston (UTHealth) School of Public Health.
According to Stephen P. Daiger, PhD, senior author of the study, an estimated 300,000 people in the U.S. suffer from the disease, which gets passed down through families.
In the study published recently in the journal Investigative Ophthalmology & Visual Science, UTHealth researchers found that in a U.S. cohort of 300 families with retinitis pigmentosa, 3 percent exhibited a mutation of the arrestin–1 gene. However, more than 36 percent of Hispanic families from the cohort exhibited the arestin–1 mutation and they all came from areas in the Southwestern U.S., such as Texas, Arizona and Southern California.
ÂWhen I started studying retinitis pigmentosa in 1985, we set out to find the Âone gene that causes the disease. Thirty–three years later, weÂve found that more than 70 genes are linked to retinitis pigmentosa, said Daiger, a professor in the Human Genetics Center and holder of the Thomas Stull Matney, PhD Professorship in Environmental and Genetic Sciences at UTHealth School of Public Health.
Some of the genes that cause retinitis pigmentosa are recessive, which means two mutations are required, and some are dominant, which means you only need one mutation. Arrestin–1 piqued DaigerÂs interest because that particular mutation is dominant while all previously found mutations in the gene are recessive. This unexpected finding shows that even a single mutation in the gene is sufficient to cause the disease.
Daiger and his team have identified the genetic cause of retinitis pigmentosa for 75 percent of families in their cohort. Possible treatments for some forms of retinitis pigmentosa are being tested but are still limited. However, the speed at which companies are developing gene therapies and small molecule therapies gives reason to hope, he said. Daiger and his collaborators have begun to connect some of the patients in the retinitis pigmentosa cohort to clinical trials that treat specific genes.
ÂI want our cohort families to know that even if there is not an immediate cure for their specific gene mutation, at this rate it wonÂt be long until a therapy becomes available, said Daiger, who also holds the Mary Farish Johnston Distinguished Chair in Ophthalmology at McGovern Medical School at UTHealth.
UTHealth coauthors include Lori S. Sullivan, PhD; Sara J. Browne, PhD; Elizabeth L. Cadena; Richard S. Ruiz, MD, and Hope Northrup, MD Additional co–authors are from Nationwide ChildrenÂs Hospital; Kellogg Eye Center at the University of Michigan; Retina Foundation of the Southwest; Casey Eye Institute at Oregon Health and Science University; Vanderbilt University and the Department of Molecular and Human Genetics at Baylor College of Medicine.
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According to Stephen P. Daiger, PhD, senior author of the study, an estimated 300,000 people in the U.S. suffer from the disease, which gets passed down through families.
In the study published recently in the journal Investigative Ophthalmology & Visual Science, UTHealth researchers found that in a U.S. cohort of 300 families with retinitis pigmentosa, 3 percent exhibited a mutation of the arrestin–1 gene. However, more than 36 percent of Hispanic families from the cohort exhibited the arestin–1 mutation and they all came from areas in the Southwestern U.S., such as Texas, Arizona and Southern California.
ÂWhen I started studying retinitis pigmentosa in 1985, we set out to find the Âone gene that causes the disease. Thirty–three years later, weÂve found that more than 70 genes are linked to retinitis pigmentosa, said Daiger, a professor in the Human Genetics Center and holder of the Thomas Stull Matney, PhD Professorship in Environmental and Genetic Sciences at UTHealth School of Public Health.
Some of the genes that cause retinitis pigmentosa are recessive, which means two mutations are required, and some are dominant, which means you only need one mutation. Arrestin–1 piqued DaigerÂs interest because that particular mutation is dominant while all previously found mutations in the gene are recessive. This unexpected finding shows that even a single mutation in the gene is sufficient to cause the disease.
Daiger and his team have identified the genetic cause of retinitis pigmentosa for 75 percent of families in their cohort. Possible treatments for some forms of retinitis pigmentosa are being tested but are still limited. However, the speed at which companies are developing gene therapies and small molecule therapies gives reason to hope, he said. Daiger and his collaborators have begun to connect some of the patients in the retinitis pigmentosa cohort to clinical trials that treat specific genes.
ÂI want our cohort families to know that even if there is not an immediate cure for their specific gene mutation, at this rate it wonÂt be long until a therapy becomes available, said Daiger, who also holds the Mary Farish Johnston Distinguished Chair in Ophthalmology at McGovern Medical School at UTHealth.
UTHealth coauthors include Lori S. Sullivan, PhD; Sara J. Browne, PhD; Elizabeth L. Cadena; Richard S. Ruiz, MD, and Hope Northrup, MD Additional co–authors are from Nationwide ChildrenÂs Hospital; Kellogg Eye Center at the University of Michigan; Retina Foundation of the Southwest; Casey Eye Institute at Oregon Health and Science University; Vanderbilt University and the Department of Molecular and Human Genetics at Baylor College of Medicine.
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