4.7 Article

Utility of red-light ultrafast optogenetic stimulation of the auditory pathway

期刊

EMBO MOLECULAR MEDICINE
卷 13, 期 6, 页码 -

出版社

WILEY
DOI: 10.15252/emmm.202013391

关键词

channelrhodopsin; cochlear implant; dynamic range; gating; spiral ganglion; temporal coding

资金

  1. European Research Council under the European Union [670759]
  2. Fraunhofer and Max-Planck cooperation program (NeurOpto grant)
  3. German Research Foundation through the Cluster of Excellence (EXC2067) Multiscale Bioimaging
  4. Leibniz Program
  5. Jacob-HenleProgramm or Else-Kroner-Fresenius-Stiftung (Promotionskolleg fur Epigenomik und Genomdynamik, 2017_Promotionskolleg.04)
  6. Fondation Pour l'Audition [FPA RD-2020-10]
  7. Projekt DEAL
  8. European Research Council (ERC) [670759] Funding Source: European Research Council (ERC)

向作者/读者索取更多资源

The study investigated the utility of fast and very fast variants of the red-light-activated ChR Chrimson for optogenetic stimulation of SGNs in mice. It was found that vf-Chrimson enabled the SGNs to fire at near-physiological rates with good temporal precision, although the light requirements were higher compared to f-Chrimson. The dynamic range of spike rate coding upon optogenetic stimulation was narrower than for acoustic clicks but larger than reported for electrical stimulation.
Optogenetic stimulation of spiral ganglion neurons (SGNs) in the ear provides a future alternative to electrical stimulation used in current cochlear implants. Here, we employed fast and very fast variants of the red-light-activated channelrhodopsin (ChR) Chrimson (f-Chrimson and vf-Chrimson) to study their utility for optogenetic stimulation of SGNs in mice. The light requirements were higher for vf-Chrimson than for f-Chrimson, even when optimizing membrane expression of vf-Chrimson by adding potassium channel trafficking sequences. Optogenetic time and intensity coding by single putative SGNs were compared with coding of acoustic clicks. vf-Chrimson enabled putative SGNs to fire at near-physiological rates with good temporal precision up to 250 Hz of stimulation. The dynamic range of SGN spike rate coding upon optogenetic stimulation was narrower than for acoustic clicks but larger than reported for electrical stimulation. The dynamic range of spike timing, on the other hand, was more comparable for optogenetic and acoustic stimulation. In conclusion, f-Chrimson and vf-Chrimson are promising candidates for optogenetic stimulation of SGNs in auditory research and future cochlear implants.

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