4.6 Article

Neuromodulation using electroosmosis

期刊

JOURNAL OF NEURAL ENGINEERING
卷 18, 期 4, 页码 -

出版社

IOP PUBLISHING LTD
DOI: 10.1088/1741-2552/ac00d3

关键词

chemical retinal stimulation; pneumatic actuation; electroosmotic flow; photoreceptor degenerative diseases; retinal prostheses; neural interface

资金

  1. National Institutes of Health [5R21EB028069-02]
  2. National Science Foundation [1840145]
  3. Directorate For Engineering
  4. Div Of Chem, Bioeng, Env, & Transp Sys [1840145] Funding Source: National Science Foundation

向作者/读者索取更多资源

The study focuses on evaluating electroosmotic flow (EOF) for delivering small quantities of glutamate to the retina as a potential strategy for treating vision loss caused by photoreceptor degenerative diseases. By constructing and testing an EOF microfluidic system, the research successfully induced excitatory and inhibitory spike rate responses in PR degenerate rat retinae, demonstrating the viability of EOF-driven chemical stimulation for retinal prosthetics.
Objective. Our laboratory has proposed chemical stimulation of retinal neurons using exogenous glutamate as a biomimetic strategy for treating vision loss caused by photoreceptor (PR) degenerative diseases. Although our previous in-vitro studies using pneumatic actuation indicate that chemical retinal stimulation is achievable, an actuation technology that is amenable to microfabrication, as needed for an in-vivo implantable device, has yet to be realized. In this study, we sought to evaluate electroosmotic flow (EOF) as a mechanism for delivering small quantities of glutamate to the retina. EOF has great potential for miniaturization. Approach. An EOF device to dispense small quantities of glutamate was constructed and its ability to drive retinal output tested in an in-vitro preparation of PR degenerate rat retina. Main results. We built and tested an EOF microfluidic system, with 3D printed and off-the-shelf components, capable of injecting small volumes of glutamate in a pulsatile fashion when a low voltage control signal was applied. With this device, we produced excitatory and inhibitory spike rate responses in PR degenerate rat retinae. Glutamate evoked spike rate responses were also observed to be voltage-dependent and localized to the site of injection. Significance. The EOF device performed similarly to a previously tested conventional pneumatic microinjector as a means of chemically stimulating the retina while eliminating the moving plunger of the pneumatic microinjector that would be difficult to miniaturize and parallelize. Although not implantable, the prototype device presented here as a proof of concept indicates that a retinal prosthetic based on EOF-driven chemical stimulation is a viable and worthwhile goal. EOF should have similar advantages for controlled dispensing of charged neurochemicals at any neural interface.

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