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Bipolar cell networks underlying steady-state intensity encoding in intrinsically photosensitive retinal ganglion cells

  • Shai Sabbah*
  • , Carin Papendorp
  • , Inbar Behrendt
  • , Hala Rasras
  • , Jesse Cann
  • , Megan L. Leyrer
  • , Elizabeth Koplas
  • , Marjo Beltoja
  • , Cameron Etebari
  • , Ali Noel Gunesch
  • , Luis Carrete
  • , Min Tae Kim
  • , Gabrielle Manoff
  • , Ananya Bhatia-Lin
  • , Tiffany Zhao
  • , Henry Dowling
  • , Kevin L. Briggman
  • , David M. Berson
  • *Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

Abstract

Intrinsically photosensitive retinal ganglion cells (ipRGCs) encode ambient light intensity at steady-state and drive physiology even in the absence of melanopsin, but the synaptic basis of such encoding remains unclear. Using ultrastructural reconstructions, we mapped specific bipolar cell (BC) types and synapses conveying photoreceptor input to ipRGCs. Functional imaging showed BC glutamate release onto ipRGCs encodes intensity at steady-state, though release onto other RGCs also exhibits such encoding. Disrupting inhibition on BCs spared intensity-encoding release at ipRGC strata but reduced it elsewhere, consistent with inhibition shifting BC dynamic range. Recording postsynaptic excitatory currents showed that ipRGCs better preserve BC-derived intensity encoding than conventional RGCs. Thus, ipRGCs receive excitation from selected, inhibition-resistant BCs whose steady-state release encodes intensity. This, together with the enhanced preservation of postsynaptic intensity encoding, ensures reliable ipRGC intensity signaling independent of visual contrast to drive physiology and behavior.

Original languageEnglish
Article number115011
JournaliScience
Volume29
Issue number3
DOIs
StatePublished - 20 Mar 2026

Bibliographical note

Publisher Copyright:
© 2026 The Author(s)

Keywords

  • cellular neuroscience
  • neuroscience
  • sensory neuroscience

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