The oxysterol 7-ketocholesterol (7KC) builds up in the body as a person ages, and in diseases including cancer and heart disease. In the eye, 7KC accumulates in Bruch’s membrane with age and in AMD—a leading cause of blindness for people over 55.
Examining the effects of 7KC in the eyes of mice, researchers found evidence that the oxysterol can effectively change choroidal endothelial cells (CECs) into cells that then invade the neural retina and lead to fibrosis. The transformed cells become enlarged lesions and fibrosis similar to those seen in poorly responsive forms of neovascular or ‘wet’ AMD, which account for 40% of poor vision in neovascular AMD. The transformed CECs may be less responsive to anti–vascular endothelial growth factor (anti-VEGF), which is the standard care for neovascular AMD.
"Any time we give anti-VEGF to a patient there can be up to a 50 percent chance they will ultimately fail treatment and have poor vision, because the patient stops responding to them long-term," explained Hartnett, a vitreoretinal surgeon and principal investigator of the study. "Of those that do not respond, 40% have fibrosis or scars. These findings provide a potential explanation for fibrosis and suggest that if we can interfere with this process, we might be able to improve outcomes in many more patients with neovascular AMD."
First author, Haibo Wang, MD PhD, added, "The results indicate an important new direction of research."
Hartnett lab authors include Haibo Wang, MD, PhD, Aniket Ramshekar, Eric Kunz and Hartnett on the research, , in the journal Angiogenesis.
The research was supported by the National Institutes of Health and an Unrestricted Grant from Research to Prevent Blindness.