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Chandelier cell anatomy and function reveal a variably distributed but common signal

Authors :
Sven Dorkenwald
Aleksandar Zlateski
Yang Li
Adam Bleckert
Ran Lu
William Wong
Jun Zhuang
Derrick Brittain
Costas A. Anastassiou
Nico Kemnitz
Shelby Suckow
Marcia C. Castro
JoAnn Buchanan
Dodam Ih
Russel Torres
Kisuk Lee
Chris S. Jordan
Brian Hu
Forrest Collman
Gayathri Mahalingam
Nicholas L. Turner
Anirban Nandi
Ignacio Tartavull
Casey M Schneider-Mizell
Emmanouil Froudarakis
Daniel J. Bumbarger
Lynne Becker
Seung Hs
Thomas Chartrand
Andreas S. Tolias
Jonathan Zung
Thomas Macrina
Robert Reid
Marc Takeno
Jacob Reimer
Jingpeng Wu
William Silversmith
Maçarico da Costa N
Agnes L. Bodor
Sergiy Popovych
Publication Year :
2020
Publisher :
Cold Spring Harbor Laboratory, 2020.

Abstract

The activity and connectivity of inhibitory cells has a profound impact on the operation of neuronal networks. While the average connectivity of many inhibitory cell types has been characterized, we still lack an understanding of how individual interneurons distribute their synapses onto their targets and how heterogeneous the inhibition is onto different individual excitatory neurons. Here, we use large-scale volumetric electron microscopy (EM) and functional imaging to address this question for chandelier cells in layer 2/3 of mouse visual cortex. Using dense morphological reconstructions from EM, we mapped the complete chandelier input onto 153 pyramidal neurons. We find that the number of input synapses is highly variable across the population, but the variability is correlated with structural features of the target neuron: soma depth, soma size, and the number of perisomatic synapses received. Functionally, we found that chandelier cell activity in vivo was highly correlated and tracks pupil diameter, a proxy for arousal state. We propose that chandelier cells provide a global signal whose strength is individually adjusted for each target neuron. This approach, combining comprehensive structural analysis with functional recordings of identified cell types, will be a powerful tool to uncover the wiring rules across the diversity of cortical cell types.

Details

Language :
English
Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....118eff5ea189b6760157ea152d98a759
Full Text :
https://doi.org/10.1101/2020.03.31.018952