February 21, 2018

Zebrafish Research Identifies Treatment Target for Eye Muscle Repair

Lab study may power new treatment to correct crossed eyes

ANN ARBOR, Mich. – By learning how zebrafish regenerate their eye muscles, researchers could help figure out how to help humans do the same. University of Michigan Kellogg Eye Center researchers have published findings in PLOS One on the role of insulin-like growth factor (IGF) in promoting extraocular muscle repair and regeneration in zebrafish.

If the process can be replicated in humans it stands to power new treatments for vision loss caused by strabismus, known as crossed eyes, and congenital ptosis, both common childhood eye diseases characterized by poorly developed eye muscles. 

Zebrafish have the unique ability to grow back damaged hearts or when they are blinded, regain the ability to see. They have become unlikely heroes in research labs around the world.

Because zebrafish share 70 percent of humans’ genetic code, it’s often possible to use them to study human genetic traits and diseases. They are assisting Kellogg researchers in basic science to regenerate the eye.

Dr. Alon Kahana
Dr. Alon Kahana

Alon Kahana, MD, PhD, an oculoplastic surgeon at U-M Kellogg Eye Center, studies the molecular mechanisms of eye muscle regeneration and the signals that regulate the regeneration process. 

For the lab study, Kahana and colleagues created a model of eye muscle dysfunction in zebrafish to study strabismus as well as congenital ptosis, the term used for droopy eyelids in children.

With strabismus, eyeglasses, exercises, or patching can help straighten the eyes and restore binocular vision, but surgery is often needed to save vision and restore function, Kahana says.

“Although humans don’t have this ability to regenerate extraocular muscle, there may be a way to enhance eye muscle repair before, during or after surgery – or maybe even to replace surgery in some cases,” says senior study author Kahana. “IGF-1 is a hormone that activates critical signaling pathways in both humans and zebrafish, and similar biology may one day provide a path toward translating our findings to clinical care.”

Kellogg authors make the case for IGF signaling as a key regulator of extraocular muscle re-growth and timing.

IGF signaling is critical for reprogramming muscle cells in the late stages of extraocular muscle regeneration, according to the study, and in the lab blocking IGF signaling diminished muscle fiber growth.

“Our fish are transparent, and the injured muscle is marked with fluorescent protein. So we can visualize the muscle repairing and growing,” says Kahana, a member of the A. Alfred Taubman Medical Research Institute. “Also because it lives in water, we can add drugs to the water to block or enhance muscle and nerve response to injury.”

The next research step is to examine the activities of the signaling pathway, and learn if the role of IGF is shared in the same reparative pathways for other muscle tissue types. 


Additional authors: Lead authorAlfonso Saera-Vila; Ke’ale W. Louie; Cuilee Sha; Ryan M. Kelly and Phillip E. Kish, all of the University of Michigan.

Citation: Extraocular muscle regeneration in zebrafish requires late signals from insulin-like growth factors. Feb. 7, 2018

Funding: This study was supported by the Alliance for Vision Research, a Physician-Scientist Award from Research to Prevent Blindness, Inc. (RPB), grant R01 EY022633 from the National Eye Institute and an unrestricted grant from RPB to the U-M Department of Ophthalmology and Visual Sciences. This research utilized the Vision Research Core, the Cancer Center Research Core, and the Michigan Diabetes Research Center at the University of Michigan.

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