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Pyramidal neurons form active, transient, multilayered circuits perturbed by autism-associated mutations at the inception of neocortex

Cortical circuits are composed predominantly of pyramidal-to-pyramidal neuron connections, yet their assembly during embryonic development is not well understood. We show that mouse embryonic Rbp4-Cre cortical neurons, transcriptomically closest to layer 5 pyramidal neurons, display two phases of ci...

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Autores principales: Munz, Martin, Bharioke, Arjun, Kosche, Georg, Moreno-Juan, Verónica, Brignall, Alexandra, Rodrigues, Tiago M., Graff-Meyer, Alexandra, Ulmer, Talia, Haeuselmann, Stephanie, Pavlinic, Dinko, Ledergerber, Nicole, Gross-Scherf, Brigitte, Rózsa, Balázs, Krol, Jacek, Picelli, Simone, Cowan, Cameron S., Roska, Botond
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cell Press 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10156177/
https://www.ncbi.nlm.nih.gov/pubmed/37071993
http://dx.doi.org/10.1016/j.cell.2023.03.025
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author Munz, Martin
Bharioke, Arjun
Kosche, Georg
Moreno-Juan, Verónica
Brignall, Alexandra
Rodrigues, Tiago M.
Graff-Meyer, Alexandra
Ulmer, Talia
Haeuselmann, Stephanie
Pavlinic, Dinko
Ledergerber, Nicole
Gross-Scherf, Brigitte
Rózsa, Balázs
Krol, Jacek
Picelli, Simone
Cowan, Cameron S.
Roska, Botond
author_facet Munz, Martin
Bharioke, Arjun
Kosche, Georg
Moreno-Juan, Verónica
Brignall, Alexandra
Rodrigues, Tiago M.
Graff-Meyer, Alexandra
Ulmer, Talia
Haeuselmann, Stephanie
Pavlinic, Dinko
Ledergerber, Nicole
Gross-Scherf, Brigitte
Rózsa, Balázs
Krol, Jacek
Picelli, Simone
Cowan, Cameron S.
Roska, Botond
author_sort Munz, Martin
collection PubMed
description Cortical circuits are composed predominantly of pyramidal-to-pyramidal neuron connections, yet their assembly during embryonic development is not well understood. We show that mouse embryonic Rbp4-Cre cortical neurons, transcriptomically closest to layer 5 pyramidal neurons, display two phases of circuit assembly in vivo. At E14.5, they form a multi-layered circuit motif, composed of only embryonic near-projecting-type neurons. By E17.5, this transitions to a second motif involving all three embryonic types, analogous to the three adult layer 5 types. In vivo patch clamp recordings and two-photon calcium imaging of embryonic Rbp4-Cre neurons reveal active somas and neurites, tetrodotoxin-sensitive voltage-gated conductances, and functional glutamatergic synapses, from E14.5 onwards. Embryonic Rbp4-Cre neurons strongly express autism-associated genes and perturbing these genes interferes with the switch between the two motifs. Hence, pyramidal neurons form active, transient, multi-layered pyramidal-to-pyramidal circuits at the inception of neocortex, and studying these circuits could yield insights into the etiology of autism.
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spelling pubmed-101561772023-05-04 Pyramidal neurons form active, transient, multilayered circuits perturbed by autism-associated mutations at the inception of neocortex Munz, Martin Bharioke, Arjun Kosche, Georg Moreno-Juan, Verónica Brignall, Alexandra Rodrigues, Tiago M. Graff-Meyer, Alexandra Ulmer, Talia Haeuselmann, Stephanie Pavlinic, Dinko Ledergerber, Nicole Gross-Scherf, Brigitte Rózsa, Balázs Krol, Jacek Picelli, Simone Cowan, Cameron S. Roska, Botond Cell Article Cortical circuits are composed predominantly of pyramidal-to-pyramidal neuron connections, yet their assembly during embryonic development is not well understood. We show that mouse embryonic Rbp4-Cre cortical neurons, transcriptomically closest to layer 5 pyramidal neurons, display two phases of circuit assembly in vivo. At E14.5, they form a multi-layered circuit motif, composed of only embryonic near-projecting-type neurons. By E17.5, this transitions to a second motif involving all three embryonic types, analogous to the three adult layer 5 types. In vivo patch clamp recordings and two-photon calcium imaging of embryonic Rbp4-Cre neurons reveal active somas and neurites, tetrodotoxin-sensitive voltage-gated conductances, and functional glutamatergic synapses, from E14.5 onwards. Embryonic Rbp4-Cre neurons strongly express autism-associated genes and perturbing these genes interferes with the switch between the two motifs. Hence, pyramidal neurons form active, transient, multi-layered pyramidal-to-pyramidal circuits at the inception of neocortex, and studying these circuits could yield insights into the etiology of autism. Cell Press 2023-04-27 /pmc/articles/PMC10156177/ /pubmed/37071993 http://dx.doi.org/10.1016/j.cell.2023.03.025 Text en © 2023 The Author(s) https://creativecommons.org/licenses/by-nc/4.0/This is an open access article under the CC BY-NC license (http://creativecommons.org/licenses/by-nc/4.0/).
spellingShingle Article
Munz, Martin
Bharioke, Arjun
Kosche, Georg
Moreno-Juan, Verónica
Brignall, Alexandra
Rodrigues, Tiago M.
Graff-Meyer, Alexandra
Ulmer, Talia
Haeuselmann, Stephanie
Pavlinic, Dinko
Ledergerber, Nicole
Gross-Scherf, Brigitte
Rózsa, Balázs
Krol, Jacek
Picelli, Simone
Cowan, Cameron S.
Roska, Botond
Pyramidal neurons form active, transient, multilayered circuits perturbed by autism-associated mutations at the inception of neocortex
title Pyramidal neurons form active, transient, multilayered circuits perturbed by autism-associated mutations at the inception of neocortex
title_full Pyramidal neurons form active, transient, multilayered circuits perturbed by autism-associated mutations at the inception of neocortex
title_fullStr Pyramidal neurons form active, transient, multilayered circuits perturbed by autism-associated mutations at the inception of neocortex
title_full_unstemmed Pyramidal neurons form active, transient, multilayered circuits perturbed by autism-associated mutations at the inception of neocortex
title_short Pyramidal neurons form active, transient, multilayered circuits perturbed by autism-associated mutations at the inception of neocortex
title_sort pyramidal neurons form active, transient, multilayered circuits perturbed by autism-associated mutations at the inception of neocortex
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10156177/
https://www.ncbi.nlm.nih.gov/pubmed/37071993
http://dx.doi.org/10.1016/j.cell.2023.03.025
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