News Release

Genetic link to dry macular degeneration found

Highlights potential risk of siRNA therapies

Peer-Reviewed Publication

University of Kentucky

LEXINGTON, Ky. (Aug. 27, 2008) – A University of Kentucky ophthalmologist, along with a team of scientists, has discovered a genetic mutation that offers protection against a type of age-related macular degeneration (AMD), a disease of the eye that is the leading cause of blindness in adults over age 50.

The study, published Wednesday in The New England Journal of Medicine, identifies a functional link between mutation of an immune-system receptor called toll-like receptor 3 (TLR3) and the "dry" type of AMD known as geographic atrophy. The untreatable, progressive disease affects an estimated 8 million Americans, causing permanent vision loss.

The discovery of the first gene associated specifically with dry AMD opens the door to developing treatments, said Dr. Jayakrishna Ambati, a retinal surgeon-scientist in UK's Department of Ophthalmology and Visual Sciences, who along with Dr. Kang Zhang, a retinal specialist and human genetics pioneer at the University of California San Diego, and Nicholas Katsanis, a molecular geneticist at The Johns Hopkins University School of Medicine, led the multi-institutional collaborative study.

Ambati's lab first discovered a relationship between a dysfunctional TLR3 mutation and decreased ocular cell toxicity in a study published in Nature earlier this year. The current study reports that TLR3 activation leads to death of specific cells in the retina and that people with the normal TLR3 gene are two to five times more likely to develop geographic atrophy than those who carry an inactive TLR3 gene mutation.

Ambati's group plans to start clinical trials next year in patients at risk for developing geographic atrophy using new TLR3 inhibitors developed in his lab.

"We finally have a potential therapy for preventing vision loss from dry AMD," Ambati said. "I am very excited by this discovery."

The study may have major preventive and therapeutic implications, according to Hemin Chin, director of the ocular genetics program at the National Eye Institute.

"Given its high prevalence in the United States and the world, finding effective prevention and treatment strategies for AMD is of critical importance," Chin said. "This finding represents a major advancement in our understanding of dry AMD, for which effective treatment is not yet available."

Of more immediate significance, an investigational drug modality known as short interfering RNA (siRNA) – currently in advanced phase trials for the "wet" type of AMD – also activates TLR3, as shown by Ambati's earlier Nature study and recently confirmed by another laboratory in the journal Nature Structural & Molecular Biology. The New England Journal of Medicine study raises the possibility that siRNA-based therapies could cause geographic atrophy.

"Collectively, these studies highlight the importance of critically assessing the potential risk posed to patients by siRNA-based therapies," Ambati said.

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Dr. Mark Kleinman and Dr. Wongil Cho, postdoctoral scholars in Ambati's lab, performed the functional studies linking TLR3 and dry AMD in human cells and animal models. Ambati's laboratory is supported by the NIH National Eye Institute, Burroughs Wellcome Fund, Research to Prevent Blindness, American Health Assistance Foundation, Macula Vision Research Foundation, and Dr. E. Vernon & Eloise C. Smith Endowed Chair. The Foundation Fighting Blindness, Macula Vision Research Foundation, Veterans Affairs Administration; and Ruth and Milton Steinbach Fund also funded this study.

Scientists from University of Utah School of Medicine, Johns Hopkins University, Sichuan Academy of Medical Sciences and Sichuan Provincial People's Hospital in Chengdu, China, Oregon Health & Science University, University of California San Diego, Greater Baltimore Medical Center, Keck School of Medicine of the University of Southern California and Rockefeller University were part of this joint effort as well.

We "see blue" at the University of Kentucky. We're home not only to powerhouse basketball and the best of intercollegiate athletics; we're also nationally ranked in more than 70 academic programs. We're charting an aggressive, exciting path toward becoming a Top 20 public research institution. "see blue." is a lot of things, but most of all it's about helping students realize their potential and harness the power of their dreams. For more about UK's efforts to become a Top 20 university and how we "see blue," visit www.uky.edu/OPBPA/business_plan.htm


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