Local politics, the county, and the world, as viewed by Tammy Maygra

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 Advances to help restore vision in humans.

 

Scientists have identified never-before-seen cells in the human eye that could potentially

help reverse vision loss caused by common diseases, such as macular degeneration. The

researchers discovered the cells in the retina, a light-sensitive structure at the back of

the eye that is vital for vision. The cells were found in donated samples of fetal tissue.

The scientists also identified the same cells in lab-grown models of the human retina — and

when they tried transplanting those models into mice with a common eye disorder, it

restored the rodents' vision.

 

The retina detects light and converts it into signals that the brain can then interpret to

determine what we're seeing. Deterioration of the retina is a leading cause of blindness

worldwide. It can be triggered by many things, including aging, diabetes and physical

injury, and the degeneration can lead to common eye diseases, such as macular degeneration

and retinitis pigmentosa.

 

Present treatments for these conditions focus mainly on reducing the rate at which retinal

cells deteriorate, and protecting those that are still healthy.  There are currently no

effective therapies that promote repair of the retina, which would effectively reverse the

deterioration.

 

A potential solution is to replace deteriorated cells with stem cells, cells that can

mature to become any type of cell in the body under the right conditions. Until now,

scientists haven't found appropriate stem cells in the human retina to accomplish this. In

the new research, the team studied the activity of cells in the fetal retinal samples in

the lab. The scientists discovered two types of retinal stem cells with promising

regenerative properties: human neural retinal stem-like cells and retinal pigment

epithelium stem-like cells.

 

The researchers found that both types of cells, which were located in the outer edge of the

retina, could clone themselves. However, only hNRSCs could turn into other types of retinal

cells under the right conditions. In a separate experiment, the researchers grew miniature

replicas of the human retina in petri dishes. These 3D tissue models, known as organoids,

better mimic the unique complexities of human organs than traditional animal models do. An

analysis of the cells within these organoids revealed that they contained hNRSCs similar to

those found in the fetal tissue samples. The team also identified specific molecular chains

of events that turned the stem cells into other retinal cells and regulated the repair

process.

 

When transplanted into the retina of mice with a disease similar to retinitis pigmentosa,

the stem cells from the organoids turned into the retinal cells needed to detect and

process light signals. These new retinal cells ultimately improved the vision of the mice,

compared with rodents that didn't receive any transplanted cells. This effect was seen for

the duration of the experiment, up to 24 weeks.

 

Taken together, these early findings suggest that hNRSCs could be used to develop new

treatments for retinal eye disorders in humans. But more research will be needed to confirm

the potential of these cells for restoring the vision of humans.

 

 

Tammy

 

 

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