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Efficient stimulation of retinal regeneration from Müller glia in adult mice using combinations of proneural bHLH transcription factors

  • Levi Todd
  • , Marcus J. Hooper
  • , Alexandra K. Haugan
  • , Connor Finkbeiner
  • , Nikolas Jorstad
  • , Nicholas Radulovich
  • , Claire K. Wong
  • , Phoebe C. Donaldson
  • , Wesley Jenkins
  • , Qiang Chen
  • , Fred Rieke
  • , Thomas A. Reh

Research output: Contribution to journalArticlepeer-review

105 Scopus citations

Abstract

Regenerative neuroscience aims to stimulate endogenous repair in the nervous system to replace neurons lost from degenerative diseases. Recently, we reported that overexpressing the transcription factor Ascl1 in Müller glia (MG) is sufficient to stimulate MG to regenerate functional neurons in the adult mouse retina. However, this process is inefficient, and only a third of the Ascl1-expressing MG generate new neurons. Here, we test whether proneural transcription factors of the Atoh1/7 class can further promote the regenerative capacity of MG. We find that the combination of Ascl1:Atoh1 is remarkably efficient at stimulating neurogenesis, even in the absence of retinal injury. Using electrophysiology and single-cell RNA sequencing (scRNA-seq), we demonstrate that Ascl1:Atoh1 generates a diversity of retinal neuron types, with the majority expressing characteristics of retinal ganglion cells. Our results provide a proof of principle that combinations of developmental transcription factors can substantially improve glial reprogramming to neurons and expand the repertoire of regenerated cell fates.

Original languageEnglish
Article number109857
JournalCell Reports
Volume37
Issue number3
DOIs
StatePublished - Oct 19 2021

Keywords

  • Muller glia
  • bHLH transcription factors
  • glia
  • regeneration
  • reprogramming
  • retina

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