Inter- and Intra-Subunit Butanol/Isoflurane Sites of Action in the Human Glycine Receptor

Glycine receptors (GlyRs) mediate inhibitory neurotransmission and are targets for alcohols and anesthetics in brain. GlyR transmembrane (TM) domains contain critical residues for alcohol/anesthetic action: amino acid A288 in TM3 forms crosslinks with TM1 (I229) in the adjacent subunit as well as TM...

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Autores principales: McCracken, Mandy L., Gorini, Giorgio, McCracken, Lindsay M., Mayfield, R. Dayne, Harris, R. Adron, Trudell, James R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2016
Materias:
Neuroscience
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4906044/
https://www.ncbi.nlm.nih.gov/pubmed/27378846
http://dx.doi.org/10.3389/fnmol.2016.00045
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author McCracken, Mandy L.
Gorini, Giorgio
McCracken, Lindsay M.
Mayfield, R. Dayne
Harris, R. Adron
Trudell, James R.
author_facet McCracken, Mandy L.
Gorini, Giorgio
McCracken, Lindsay M.
Mayfield, R. Dayne
Harris, R. Adron
Trudell, James R.
author_sort McCracken, Mandy L.
collection PubMed
description Glycine receptors (GlyRs) mediate inhibitory neurotransmission and are targets for alcohols and anesthetics in brain. GlyR transmembrane (TM) domains contain critical residues for alcohol/anesthetic action: amino acid A288 in TM3 forms crosslinks with TM1 (I229) in the adjacent subunit as well as TM2 (S267) and TM4 (Y406, W407, I409, Y410) in the same subunit. We hypothesized that these residues may participate in intra-subunit and inter-subunit sites of alcohol/anesthetic action. The following double and triple mutants of GLRA1 cDNA (encoding human glycine receptor alpha 1 subunit) were injected into Xenopus laevis oocytes: I229C/A288C, I229C/A288C/C290S, A288C/Y406C, A288C/W407C, A288C/I409C, and A288C/Y410C along with the corresponding single mutants and wild-type GLRA1. Butanol (22 mM) or isoflurane (0.6 mM) potentiation of GlyR-mediated currents before and after application of the cysteine crosslinking agent HgCl(2) (10 μM) was measured using two-electrode voltage clamp electrophysiology. Crosslinking nearly abolished butanol and isoflurane potentiation in the I229C/A288C and I229C/A288C/C290S mutants but had no effect in single mutants or wild-type. Crosslinking also inhibited butanol and isoflurane potentiation in the TM3-4 mutants (A288C/Y406C, A288C/W407C, A288C/I409C, A288C/Y410C) with no effect in single mutants or wild-type. We extracted proteins from oocytes expressing I229C/288C, A288C/Y410C, or wild-type GlyRs, used mass spectrometry to verify their expression and possible inter-subunit dimerization, plus immunoblotting to investigate the biochemical features of proposed crosslinks. Wild-type GlyR subunits measured about 50 kDa; after crosslinking, the dimeric/monomeric 100:50 kDa band ratio was significantly increased in I229C/288C but not A288C/Y410C mutants or wild-type, providing support for TM1-3 inter-subunit and TM3-4 intra-subunit crosslinking. A GlyR homology model based on the GluCl template provides further evidence for a multi-site model for alcohol/anesthetic interaction with human GLRA1.
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spelling pubmed-49060442016-07-04 Inter- and Intra-Subunit Butanol/Isoflurane Sites of Action in the Human Glycine Receptor McCracken, Mandy L. Gorini, Giorgio McCracken, Lindsay M. Mayfield, R. Dayne Harris, R. Adron Trudell, James R. Front Mol Neurosci Neuroscience Glycine receptors (GlyRs) mediate inhibitory neurotransmission and are targets for alcohols and anesthetics in brain. GlyR transmembrane (TM) domains contain critical residues for alcohol/anesthetic action: amino acid A288 in TM3 forms crosslinks with TM1 (I229) in the adjacent subunit as well as TM2 (S267) and TM4 (Y406, W407, I409, Y410) in the same subunit. We hypothesized that these residues may participate in intra-subunit and inter-subunit sites of alcohol/anesthetic action. The following double and triple mutants of GLRA1 cDNA (encoding human glycine receptor alpha 1 subunit) were injected into Xenopus laevis oocytes: I229C/A288C, I229C/A288C/C290S, A288C/Y406C, A288C/W407C, A288C/I409C, and A288C/Y410C along with the corresponding single mutants and wild-type GLRA1. Butanol (22 mM) or isoflurane (0.6 mM) potentiation of GlyR-mediated currents before and after application of the cysteine crosslinking agent HgCl(2) (10 μM) was measured using two-electrode voltage clamp electrophysiology. Crosslinking nearly abolished butanol and isoflurane potentiation in the I229C/A288C and I229C/A288C/C290S mutants but had no effect in single mutants or wild-type. Crosslinking also inhibited butanol and isoflurane potentiation in the TM3-4 mutants (A288C/Y406C, A288C/W407C, A288C/I409C, A288C/Y410C) with no effect in single mutants or wild-type. We extracted proteins from oocytes expressing I229C/288C, A288C/Y410C, or wild-type GlyRs, used mass spectrometry to verify their expression and possible inter-subunit dimerization, plus immunoblotting to investigate the biochemical features of proposed crosslinks. Wild-type GlyR subunits measured about 50 kDa; after crosslinking, the dimeric/monomeric 100:50 kDa band ratio was significantly increased in I229C/288C but not A288C/Y410C mutants or wild-type, providing support for TM1-3 inter-subunit and TM3-4 intra-subunit crosslinking. A GlyR homology model based on the GluCl template provides further evidence for a multi-site model for alcohol/anesthetic interaction with human GLRA1. Frontiers Media S.A. 2016-06-14 /pmc/articles/PMC4906044/ /pubmed/27378846 http://dx.doi.org/10.3389/fnmol.2016.00045 Text en Copyright © 2016 McCracken, Gorini, McCracken, Mayfield, Harris and Trudell. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Neuroscience
McCracken, Mandy L.
Gorini, Giorgio
McCracken, Lindsay M.
Mayfield, R. Dayne
Harris, R. Adron
Trudell, James R.
Inter- and Intra-Subunit Butanol/Isoflurane Sites of Action in the Human Glycine Receptor
title Inter- and Intra-Subunit Butanol/Isoflurane Sites of Action in the Human Glycine Receptor
title_full Inter- and Intra-Subunit Butanol/Isoflurane Sites of Action in the Human Glycine Receptor
title_fullStr Inter- and Intra-Subunit Butanol/Isoflurane Sites of Action in the Human Glycine Receptor
title_full_unstemmed Inter- and Intra-Subunit Butanol/Isoflurane Sites of Action in the Human Glycine Receptor
title_short Inter- and Intra-Subunit Butanol/Isoflurane Sites of Action in the Human Glycine Receptor
title_sort inter- and intra-subunit butanol/isoflurane sites of action in the human glycine receptor
topic Neuroscience
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4906044/
https://www.ncbi.nlm.nih.gov/pubmed/27378846
http://dx.doi.org/10.3389/fnmol.2016.00045
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