WASHINGTON U. - ST. LOUIS (US) - Good vision depends, at least in part, on a recycling process in the eye that mops up cellular debris and reuses light-sensitive proteins.
Disruptions in that process may harm vision and play a key role in the development of eye diseases related to aging, including age-related macular degeneration, the leading cause of vision loss in Americans over 50.
In the brain, similar defects in the recycling of proteins contribute to other disorders associated with aging, such as Alzheimer's and Parkinson's diseases, both of which are linked to the build up and aggregation of proteins in brain cells.
"One possibility is that as we age, these recycling pathways can become less efficient and the system becomes clogged," says co-senior author Thomas A. Ferguson, a professor of ophthalmology and visual sciences at Washington University in St. Louis.
"That can cut down on the retina's ability to use vitamin A, which is crucial to good vision. Inefficient recycling also is thought to contribute to disorders like Alzheimer's, where patients can't clear proteins from the brain as they get older."
Working with mice, researchers showed that vision suffers when the retina can't clear away debris produced by light-sensing photoreceptor cells.
The retina, located at the back of the eye, is populated with photoreceptors that absorb light and send electrical signals to the brain, allowing us to see. A key component of these photoreceptors is a light-sensitive molecule called rhodopsin.
It is rhodopsin that absorbs light, but each rhodopsin molecule only works for a brief stint. Once it has been exposed to light, rhodopsin breaks down and must be recycled to use again.
"After rhodopsin absorbs light, it's no good anymore," Ferguson says. "But the 'spent' rhodopsin is recharged through a series of chemical reactions so that the whole process can start all over again."
The key player in getting the rhodopsin recharged is a single layer of cells at the back of the retina called the retinal pigment epithelium (RPE), which recycles and recharges a molecule that rhodopsin needs to activate the photoreceptor cells.
In addition, the photoreceptor cells themselves also get a little ragged after repeated exposure to light and they, too, are continually shed and renewed each day.
Survival mechanism
In this new study, published in the journal researchers found that both the recycling of rhodopsin and the clearance of discarded bits of photoreceptors are initiated by a mechanism called autophagy.
"Autophagy is just what it sounds like: self-eating," says Douglas Green, the chair of immunology at St. Jude Children's Research Hospital. "Under adverse conditions, cells digest their own internal structures. They essentially eat themselves to survive. The process we've studied shares features of autophagy, but also is distinct, and that's very exciting."
There is increasing evidence that when operating efficiently, autophagy can help stave off the cellular damage that occurs in age-related diseases such as Alzheimer's, and researchers suspect it also may play a role in age-related eye diseases.
But autophagy isn't the only mechanism at work in the retina. The retinal pigment epithelium (RPE) also uses a second eating process called phagocytosis to clear away parts of the photoreceptor cells that are constantly shed in the retina.
But it turns out that both autophagy-when cells eat themselves-and phagocytosis-when cells eat structures other than themselves-operate through the same pathway, the research shows.
Interrupted pathway
To understand how those two mechanisms operate in the eye, Ferguson and Green studied mice. In the animals, as in people, photoreceptor discs are shed early each morning. The researchers found that signs of autophagy were visible in the mouse retina throughout the day but peaked at about 7 a.m.
Next, they generated mice whose retinal pigment epithelial cells lacked a gene essential for autophagy.
"One of the first things we noticed was that disrupting this unusual form of autophagy also disrupted the process of phagocytosis," Green explains. "The retinal pigment epithelium cells weren't able to digest debris from photoreceptors, suggesting that the two mechanisms shared a common pathway in the retina."
They also found that when the pathway was interrupted, the mice didn't see very well. Using complex techniques to measure vision, the researchers discovered that although the mice weren't losing photoreceptor cells, they were losing their vision.
"Their vision was reduced by 30 to 40 percent," Ferguson says. "But when we gave each of the mice a single injection of a molecule to restore the rhodopsin in their photoreceptors, their vision was restored to normal for several days."
Vitamin A
The experiments suggest that autophagy assists the visual cycle by helping cells recover vitamin A, which is essential for the recycling of rhodopsin in the photoreceptors.
"And that is very interesting because deficiencies in vitamin A are known to lead to night blindness and other vision problems," Ferguson says. "We can't really say these mice were 'night blind,' but their vision was reduced because they couldn't efficiently recover enough vitamin A to restore rhodopsin to the photoreceptors."
If that same process were to break down in humans as a function of aging, Ferguson believes it could play a role in the vision loss associated with normal aging and with diseases like macular degeneration.
"If autophagy becomes less efficient in the retina as a result of aging, it could cause problems clearing away debris and maintaining the visual cycle," he says.
Because previous studies have suggested autophagy can help clear harmful proteins that accumulate in cells during Alzheimer's and Parkinson's disease, new drugs are being developed to boost that recycling process. Ferguson and Green think some of those drugs may be useful in combating age-related vision loss.
Funding for this research comes from the National Eye Institute, the National Institute of Allergy and Infectious Diseases of the National Institutes of Health, and by Research to Prevent Blindness and the BrightFocus Foundation.
Source: Washington University in St. Louis
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