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A photoswitchable GABA receptor channel blocker

BACKGROUND AND PURPOSE: Anion‐selective Cys‐loop receptors (GABA and glycine receptors) provide the main inhibitory drive in the CNS. Both types of receptor operate via chloride‐selective ion channels, though with different kinetics, pharmacological profiles, and localization. Disequilibrium in thei...

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Autores principales: Maleeva, Galyna, Wutz, Daniel, Rustler, Karin, Nin‐Hill, Alba, Rovira, Carme, Petukhova, Elena, Bautista‐Barrufet, Antoni, Gomila‐Juaneda, Alexandre, Scholze, Petra, Peiretti, Franck, Alfonso‐Prieto, Mercedes, König, Burkhard, Gorostiza, Pau, Bregestovski, Piotr
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6609548/
https://www.ncbi.nlm.nih.gov/pubmed/30981211
http://dx.doi.org/10.1111/bph.14689
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author Maleeva, Galyna
Wutz, Daniel
Rustler, Karin
Nin‐Hill, Alba
Rovira, Carme
Petukhova, Elena
Bautista‐Barrufet, Antoni
Gomila‐Juaneda, Alexandre
Scholze, Petra
Peiretti, Franck
Alfonso‐Prieto, Mercedes
König, Burkhard
Gorostiza, Pau
Bregestovski, Piotr
author_facet Maleeva, Galyna
Wutz, Daniel
Rustler, Karin
Nin‐Hill, Alba
Rovira, Carme
Petukhova, Elena
Bautista‐Barrufet, Antoni
Gomila‐Juaneda, Alexandre
Scholze, Petra
Peiretti, Franck
Alfonso‐Prieto, Mercedes
König, Burkhard
Gorostiza, Pau
Bregestovski, Piotr
author_sort Maleeva, Galyna
collection PubMed
description BACKGROUND AND PURPOSE: Anion‐selective Cys‐loop receptors (GABA and glycine receptors) provide the main inhibitory drive in the CNS. Both types of receptor operate via chloride‐selective ion channels, though with different kinetics, pharmacological profiles, and localization. Disequilibrium in their function leads to a variety of disorders, which are often treated with allosteric modulators. The few available GABA and glycine receptor channel blockers effectively suppress inhibitory currents in neurons, but their systemic administration is highly toxic. With the aim of developing an efficient light‐controllable modulator of GABA receptors, we constructed azobenzene‐nitrazepam (Azo‐NZ1), which is composed of a nitrazepam moiety merged to an azobenzene photoisomerizable group. EXPERIMENTAL APPROACH: The experiments were carried out on cultured cells expressing Cys‐loop receptors of known subunit composition and in brain slices using patch‐clamp. Site‐directed mutagenesis and molecular modelling approaches were applied to evaluate the mechanism of action of Azo‐NZ1. KEY RESULTS: At visible light, being in trans‐configuration, Azo‐NZ1 blocked heteromeric α1/β2/γ2 GABA(A) receptors, ρ2 GABA(A) (GABA(C)), and α2 glycine receptors, whereas switching the compound into cis‐state by UV illumination restored the activity. Azo‐NZ1 successfully photomodulated GABAergic currents recorded from dentate gyrus neurons. We demonstrated that in trans‐configuration, Azo‐NZ1 blocks the Cl‐selective ion pore of GABA receptors interacting mainly with the 2′ level of the TM2 region. CONCLUSIONS AND IMPLICATIONS: Azo‐NZ1 is a soluble light‐driven Cl‐channel blocker, which allows photo‐modulation of the activity induced by anion‐selective Cys‐loop receptors. Azo‐NZ1 is able to control GABAergic postsynaptic currents and provides new opportunities to study inhibitory neurotransmission using patterned illumination.
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spelling pubmed-66095482019-07-09 A photoswitchable GABA receptor channel blocker Maleeva, Galyna Wutz, Daniel Rustler, Karin Nin‐Hill, Alba Rovira, Carme Petukhova, Elena Bautista‐Barrufet, Antoni Gomila‐Juaneda, Alexandre Scholze, Petra Peiretti, Franck Alfonso‐Prieto, Mercedes König, Burkhard Gorostiza, Pau Bregestovski, Piotr Br J Pharmacol Research Papers BACKGROUND AND PURPOSE: Anion‐selective Cys‐loop receptors (GABA and glycine receptors) provide the main inhibitory drive in the CNS. Both types of receptor operate via chloride‐selective ion channels, though with different kinetics, pharmacological profiles, and localization. Disequilibrium in their function leads to a variety of disorders, which are often treated with allosteric modulators. The few available GABA and glycine receptor channel blockers effectively suppress inhibitory currents in neurons, but their systemic administration is highly toxic. With the aim of developing an efficient light‐controllable modulator of GABA receptors, we constructed azobenzene‐nitrazepam (Azo‐NZ1), which is composed of a nitrazepam moiety merged to an azobenzene photoisomerizable group. EXPERIMENTAL APPROACH: The experiments were carried out on cultured cells expressing Cys‐loop receptors of known subunit composition and in brain slices using patch‐clamp. Site‐directed mutagenesis and molecular modelling approaches were applied to evaluate the mechanism of action of Azo‐NZ1. KEY RESULTS: At visible light, being in trans‐configuration, Azo‐NZ1 blocked heteromeric α1/β2/γ2 GABA(A) receptors, ρ2 GABA(A) (GABA(C)), and α2 glycine receptors, whereas switching the compound into cis‐state by UV illumination restored the activity. Azo‐NZ1 successfully photomodulated GABAergic currents recorded from dentate gyrus neurons. We demonstrated that in trans‐configuration, Azo‐NZ1 blocks the Cl‐selective ion pore of GABA receptors interacting mainly with the 2′ level of the TM2 region. CONCLUSIONS AND IMPLICATIONS: Azo‐NZ1 is a soluble light‐driven Cl‐channel blocker, which allows photo‐modulation of the activity induced by anion‐selective Cys‐loop receptors. Azo‐NZ1 is able to control GABAergic postsynaptic currents and provides new opportunities to study inhibitory neurotransmission using patterned illumination. John Wiley and Sons Inc. 2019-06-26 2019-08 /pmc/articles/PMC6609548/ /pubmed/30981211 http://dx.doi.org/10.1111/bph.14689 Text en © 2019 Institut de Neurosciences des Systémes. British Journal of Pharmacology published by John Wiley & Sons Ltd on behalf of British Pharmacological Society. This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited and is not used for commercial purposes.
spellingShingle Research Papers
Maleeva, Galyna
Wutz, Daniel
Rustler, Karin
Nin‐Hill, Alba
Rovira, Carme
Petukhova, Elena
Bautista‐Barrufet, Antoni
Gomila‐Juaneda, Alexandre
Scholze, Petra
Peiretti, Franck
Alfonso‐Prieto, Mercedes
König, Burkhard
Gorostiza, Pau
Bregestovski, Piotr
A photoswitchable GABA receptor channel blocker
title A photoswitchable GABA receptor channel blocker
title_full A photoswitchable GABA receptor channel blocker
title_fullStr A photoswitchable GABA receptor channel blocker
title_full_unstemmed A photoswitchable GABA receptor channel blocker
title_short A photoswitchable GABA receptor channel blocker
title_sort photoswitchable gaba receptor channel blocker
topic Research Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6609548/
https://www.ncbi.nlm.nih.gov/pubmed/30981211
http://dx.doi.org/10.1111/bph.14689
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