4.6 Article

A Microfluidic Eye Facsimile System to Examine the Migration of Stem-like Cells

期刊

MICROMACHINES
卷 13, 期 3, 页码 -

出版社

MDPI
DOI: 10.3390/mi13030406

关键词

electric fields; chemotaxis; retina; transplantation

资金

  1. US National Institutes of Health [NEI 1R21 EY031439-01]

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Millions of adults worldwide are affected by progressive vision loss. Current cell replacement therapies face a challenge of inability to migrate to targeted areas. A bioengineering system called mu-Eye has been developed to stimulate and examine the migration of retinal stem cells (SCs) within eye facsimiles using external stimuli, showing promising results for promoting migration-targeted strategies for retinal cell replacement therapy.
Millions of adults are affected by progressive vision loss worldwide. The rising incidence of retinal diseases can be attributed to damage or degeneration of neurons that convert light into electrical signals for vision. Contemporary cell replacement therapies have transplanted stem and progenitor-like cells (SCs) into adult retinal tissue to replace damaged neurons and restore the visual neural network. However, the inability of SCs to migrate to targeted areas remains a fundamental challenge. Current bioengineering projects aim to integrate microfluidic technologies with organotypic cultures to examine SC behaviors within biomimetic environments. The application of neural phantoms, or eye facsimiles, in such systems will greatly aid the study of SC migratory behaviors in 3D. This project developed a bioengineering system, called the mu-Eye, to stimulate and examine the migration of retinal SCs within eye facsimiles using external chemical and electrical stimuli. Results illustrate that the imposed fields stimulated large, directional SC migration into eye facsimiles, and that electro-chemotactic stimuli produced significantly larger increases in cell migration than the individual stimuli combined. These findings highlight the significance of microfluidic systems in the development of approaches that apply external fields for neural repair and promote migration-targeted strategies for retinal cell replacement therapy.

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