Auxiliary α2δ1 and α2δ3 Subunits of Calcium Channels Drive Excitatory and Inhibitory Neuronal Network Development

VGCCs are multisubunit complexes that play a crucial role in neuronal signaling. Auxiliary α2δ subunits of VGCCs modulate trafficking and biophysical properties of the pore-forming α1 subunit and trigger excitatory synaptogenesis. Alterations in the expression level of α2δ subunits were implicated i...

Descripción completa

Detalles Bibliográficos
Autores principales: Bikbaev, Arthur, Ciuraszkiewicz-Wojciech, Anna, Heck, Jennifer, Klatt, Oliver, Freund, Romy, Mitlöhner, Jessica, Enrile Lacalle, Sara, Sun, Miao, Repetto, Daniele, Frischknecht, Renato, Ablinger, Cornelia, Rohlmann, Astrid, Missler, Markus, Obermair, Gerald J., Di Biase, Valentina, Heine, Martin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Society for Neuroscience 2020
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7326358/
https://www.ncbi.nlm.nih.gov/pubmed/32414783
http://dx.doi.org/10.1523/JNEUROSCI.1707-19.2020
_version_ 1783552326938656768
author Bikbaev, Arthur
Ciuraszkiewicz-Wojciech, Anna
Heck, Jennifer
Klatt, Oliver
Freund, Romy
Mitlöhner, Jessica
Enrile Lacalle, Sara
Sun, Miao
Repetto, Daniele
Frischknecht, Renato
Ablinger, Cornelia
Rohlmann, Astrid
Missler, Markus
Obermair, Gerald J.
Di Biase, Valentina
Heine, Martin
author_facet Bikbaev, Arthur
Ciuraszkiewicz-Wojciech, Anna
Heck, Jennifer
Klatt, Oliver
Freund, Romy
Mitlöhner, Jessica
Enrile Lacalle, Sara
Sun, Miao
Repetto, Daniele
Frischknecht, Renato
Ablinger, Cornelia
Rohlmann, Astrid
Missler, Markus
Obermair, Gerald J.
Di Biase, Valentina
Heine, Martin
author_sort Bikbaev, Arthur
collection PubMed
description VGCCs are multisubunit complexes that play a crucial role in neuronal signaling. Auxiliary α2δ subunits of VGCCs modulate trafficking and biophysical properties of the pore-forming α1 subunit and trigger excitatory synaptogenesis. Alterations in the expression level of α2δ subunits were implicated in several syndromes and diseases, including chronic neuropathic pain, autism, and epilepsy. However, the contribution of distinct α2δ subunits to excitatory/inhibitory imbalance and aberrant network connectivity characteristic for these pathologic conditions remains unclear. Here, we show that α2δ1 overexpression enhances spontaneous neuronal network activity in developing and mature cultures of hippocampal neurons. In contrast, overexpression, but not downregulation, of α2δ3 enhances neuronal firing in immature cultures, whereas later in development it suppresses neuronal activity. We found that α2δ1 overexpression increases excitatory synaptic density and selectively enhances presynaptic glutamate release, which is impaired on α2δ1 knockdown. Overexpression of α2δ3 increases the excitatory synaptic density as well but also facilitates spontaneous GABA release and triggers an increase in the density of inhibitory synapses, which is accompanied by enhanced axonaloutgrowth in immature interneurons. Together, our findings demonstrate that α2δ1 and α2δ3 subunits play distinct but complementary roles in driving formation of structural and functional network connectivity during early development. An alteration in α2δ surface expression during critical developmental windows can therefore play a causal role and have a profound impact on the excitatory-to-inhibitory balance and network connectivity. SIGNIFICANCE STATEMENT The computational capacity of neuronal networks is determined by their connectivity. Chemical synapses are the main interface for transfer of information between individual neurons. The initial formation of network connectivity requires spontaneous electrical activity and the calcium channel-mediated signaling. We found that, in early development, auxiliary α2δ3 subunits of calcium channels foster presynaptic release of GABA, trigger formation of inhibitory synapses, and promote axonal outgrowth in inhibitory interneurons. In contrast, later in development, α2δ1 subunits promote the glutamatergic neurotransmission and synaptogenesis, as well as strongly enhance neuronal network activity. We propose that formation of connectivity in neuronal networks is associated with a concerted interplay of α2δ1 and α2δ3 subunits of calcium channels.
format Online
Article
Text
id pubmed-7326358
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Society for Neuroscience
record_format MEDLINE/PubMed
spelling pubmed-73263582020-07-01 Auxiliary α2δ1 and α2δ3 Subunits of Calcium Channels Drive Excitatory and Inhibitory Neuronal Network Development Bikbaev, Arthur Ciuraszkiewicz-Wojciech, Anna Heck, Jennifer Klatt, Oliver Freund, Romy Mitlöhner, Jessica Enrile Lacalle, Sara Sun, Miao Repetto, Daniele Frischknecht, Renato Ablinger, Cornelia Rohlmann, Astrid Missler, Markus Obermair, Gerald J. Di Biase, Valentina Heine, Martin J Neurosci Research Articles VGCCs are multisubunit complexes that play a crucial role in neuronal signaling. Auxiliary α2δ subunits of VGCCs modulate trafficking and biophysical properties of the pore-forming α1 subunit and trigger excitatory synaptogenesis. Alterations in the expression level of α2δ subunits were implicated in several syndromes and diseases, including chronic neuropathic pain, autism, and epilepsy. However, the contribution of distinct α2δ subunits to excitatory/inhibitory imbalance and aberrant network connectivity characteristic for these pathologic conditions remains unclear. Here, we show that α2δ1 overexpression enhances spontaneous neuronal network activity in developing and mature cultures of hippocampal neurons. In contrast, overexpression, but not downregulation, of α2δ3 enhances neuronal firing in immature cultures, whereas later in development it suppresses neuronal activity. We found that α2δ1 overexpression increases excitatory synaptic density and selectively enhances presynaptic glutamate release, which is impaired on α2δ1 knockdown. Overexpression of α2δ3 increases the excitatory synaptic density as well but also facilitates spontaneous GABA release and triggers an increase in the density of inhibitory synapses, which is accompanied by enhanced axonaloutgrowth in immature interneurons. Together, our findings demonstrate that α2δ1 and α2δ3 subunits play distinct but complementary roles in driving formation of structural and functional network connectivity during early development. An alteration in α2δ surface expression during critical developmental windows can therefore play a causal role and have a profound impact on the excitatory-to-inhibitory balance and network connectivity. SIGNIFICANCE STATEMENT The computational capacity of neuronal networks is determined by their connectivity. Chemical synapses are the main interface for transfer of information between individual neurons. The initial formation of network connectivity requires spontaneous electrical activity and the calcium channel-mediated signaling. We found that, in early development, auxiliary α2δ3 subunits of calcium channels foster presynaptic release of GABA, trigger formation of inhibitory synapses, and promote axonal outgrowth in inhibitory interneurons. In contrast, later in development, α2δ1 subunits promote the glutamatergic neurotransmission and synaptogenesis, as well as strongly enhance neuronal network activity. We propose that formation of connectivity in neuronal networks is associated with a concerted interplay of α2δ1 and α2δ3 subunits of calcium channels. Society for Neuroscience 2020-06-17 /pmc/articles/PMC7326358/ /pubmed/32414783 http://dx.doi.org/10.1523/JNEUROSCI.1707-19.2020 Text en Copyright © 2020 Bikbaev, Ciuraszkiewicz-Wojciech et al. https://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License Creative Commons Attribution 4.0 International (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed.
spellingShingle Research Articles
Bikbaev, Arthur
Ciuraszkiewicz-Wojciech, Anna
Heck, Jennifer
Klatt, Oliver
Freund, Romy
Mitlöhner, Jessica
Enrile Lacalle, Sara
Sun, Miao
Repetto, Daniele
Frischknecht, Renato
Ablinger, Cornelia
Rohlmann, Astrid
Missler, Markus
Obermair, Gerald J.
Di Biase, Valentina
Heine, Martin
Auxiliary α2δ1 and α2δ3 Subunits of Calcium Channels Drive Excitatory and Inhibitory Neuronal Network Development
title Auxiliary α2δ1 and α2δ3 Subunits of Calcium Channels Drive Excitatory and Inhibitory Neuronal Network Development
title_full Auxiliary α2δ1 and α2δ3 Subunits of Calcium Channels Drive Excitatory and Inhibitory Neuronal Network Development
title_fullStr Auxiliary α2δ1 and α2δ3 Subunits of Calcium Channels Drive Excitatory and Inhibitory Neuronal Network Development
title_full_unstemmed Auxiliary α2δ1 and α2δ3 Subunits of Calcium Channels Drive Excitatory and Inhibitory Neuronal Network Development
title_short Auxiliary α2δ1 and α2δ3 Subunits of Calcium Channels Drive Excitatory and Inhibitory Neuronal Network Development
title_sort auxiliary α2δ1 and α2δ3 subunits of calcium channels drive excitatory and inhibitory neuronal network development
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7326358/
https://www.ncbi.nlm.nih.gov/pubmed/32414783
http://dx.doi.org/10.1523/JNEUROSCI.1707-19.2020
work_keys_str_mv AT bikbaevarthur auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT ciuraszkiewiczwojciechanna auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT heckjennifer auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT klattoliver auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT freundromy auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT mitlohnerjessica auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT enrilelacallesara auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT sunmiao auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT repettodaniele auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT frischknechtrenato auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT ablingercornelia auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT rohlmannastrid auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT misslermarkus auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT obermairgeraldj auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT dibiasevalentina auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment
AT heinemartin auxiliarya2d1anda2d3subunitsofcalciumchannelsdriveexcitatoryandinhibitoryneuronalnetworkdevelopment

Ejemplares similares