The relationship between glycine receptor agonist efficacy and allosteric modulation

The relationship between glycine receptor agonist efficacy and allosteric modulation

Show other versions (1)

The glycine receptor (GlyR) is a ligand-gated ion channel member of the cys-loop receptor superfamily, responsible for inhibitory neurotransmission in the brain and spinal cord. Both glycine and the partial agonist taurine act as endogenous ligands of the GlyR. Taurine-activated GlyR may have a role...

Full description

Bibliographic Details
Main Author: Kirson, Dean
Format: Others
Language:en
Published: 2014
Subjects:
Glycine receptor
Glycine
Taurine
Alcohol
Anesthetic
Inhalant
Zinc
Partial agonist
Agonist
Efficacy
Allosteric modulation
Single channel
Electrophysiology
Online Access:http://hdl.handle.net/2152/24808
id ndltd-UTEXAS-oai-repositories.lib.utexas.edu-2152-24808
record_format oai_dc
spelling ndltd-UTEXAS-oai-repositories.lib.utexas.edu-2152-248082015-09-20T17:23:23ZThe relationship between glycine receptor agonist efficacy and allosteric modulationKirson, DeanGlycine receptorGlycineTaurineAlcoholAnestheticInhalantZincPartial agonistAgonistEfficacyAllosteric modulationSingle channelElectrophysiologyThe glycine receptor (GlyR) is a ligand-gated ion channel member of the cys-loop receptor superfamily, responsible for inhibitory neurotransmission in the brain and spinal cord. Both glycine and the partial agonist taurine act as endogenous ligands of the GlyR. Taurine-activated GlyR may have a role in the rewarding effects of drugs of abuse, such as ethanol. As a partial agonist, taurine has a decreased efficacy relative to glycine, resulting in a decreased maximum response. We investigated the effects of ethanol, anesthetics, inhalants, and zinc to determine if these allosteric modulators could increase the efficacy of the taurine-activated GlyR. Whole cell recordings of wild type GlyR revealed that each of the allosteric modulators potentiated currents generated by saturating concentrations of taurine but not glycine, implying an increase in efficacy. Zinc is found at GlyR-potentiating concentrations throughout the nervous system, so we examined the combinatorial effects of these allosteric modulators with zinc to mimic in vivo conditions. Whole cell recordings revealed that zinc potentiation of saturating taurine-generated currents decreased further potentiation by another allosteric modulator, indicating no synergistic effects on efficacy. We next investigated the actions of ethanol and isoflurane on the taurine-activated GlyR at the single channel level, finding that both allosteric modulators stabilized the channel open state, increasing the efficacy of the taurine-activated GlyR. We previously identified a mutation in the ligand-binding domain of the GlyR (D97R) that produces spontaneously activating channels, on which taurine has increased efficacy. We identified a residue, R131, as a possible binding partner of D97 in forming an electrostatic interaction that holds the channel in the closed state. We found that disruption of this interaction results in greatly increased taurine efficacy, indicating that efficacy for partial agonists may be determined by agonist ability to break this bond early in the activation process following binding. Thus we find differential mechanisms of allosteric modulation and efficacy determinations for the GlyR when activated by taurine vs. glycine.text2014-06-25T14:54:41Z2014-052014-05-30May 20142014-06-25T14:54:41ZThesisapplication/pdfhttp://hdl.handle.net/2152/24808en
collection NDLTD
language en
format Others
sources NDLTD
topic Glycine receptor
Glycine
Taurine
Alcohol
Anesthetic
Inhalant
Zinc
Partial agonist
Agonist
Efficacy
Allosteric modulation
Single channel
Electrophysiology
spellingShingle Glycine receptor
Glycine
Taurine
Alcohol
Anesthetic
Inhalant
Zinc
Partial agonist
Agonist
Efficacy
Allosteric modulation
Single channel
Electrophysiology
Kirson, Dean
The relationship between glycine receptor agonist efficacy and allosteric modulation
description The glycine receptor (GlyR) is a ligand-gated ion channel member of the cys-loop receptor superfamily, responsible for inhibitory neurotransmission in the brain and spinal cord. Both glycine and the partial agonist taurine act as endogenous ligands of the GlyR. Taurine-activated GlyR may have a role in the rewarding effects of drugs of abuse, such as ethanol. As a partial agonist, taurine has a decreased efficacy relative to glycine, resulting in a decreased maximum response. We investigated the effects of ethanol, anesthetics, inhalants, and zinc to determine if these allosteric modulators could increase the efficacy of the taurine-activated GlyR. Whole cell recordings of wild type GlyR revealed that each of the allosteric modulators potentiated currents generated by saturating concentrations of taurine but not glycine, implying an increase in efficacy. Zinc is found at GlyR-potentiating concentrations throughout the nervous system, so we examined the combinatorial effects of these allosteric modulators with zinc to mimic in vivo conditions. Whole cell recordings revealed that zinc potentiation of saturating taurine-generated currents decreased further potentiation by another allosteric modulator, indicating no synergistic effects on efficacy. We next investigated the actions of ethanol and isoflurane on the taurine-activated GlyR at the single channel level, finding that both allosteric modulators stabilized the channel open state, increasing the efficacy of the taurine-activated GlyR. We previously identified a mutation in the ligand-binding domain of the GlyR (D97R) that produces spontaneously activating channels, on which taurine has increased efficacy. We identified a residue, R131, as a possible binding partner of D97 in forming an electrostatic interaction that holds the channel in the closed state. We found that disruption of this interaction results in greatly increased taurine efficacy, indicating that efficacy for partial agonists may be determined by agonist ability to break this bond early in the activation process following binding. Thus we find differential mechanisms of allosteric modulation and efficacy determinations for the GlyR when activated by taurine vs. glycine. === text
author Kirson, Dean
author_facet Kirson, Dean
author_sort Kirson, Dean
title The relationship between glycine receptor agonist efficacy and allosteric modulation
title_short The relationship between glycine receptor agonist efficacy and allosteric modulation
title_full The relationship between glycine receptor agonist efficacy and allosteric modulation
title_fullStr The relationship between glycine receptor agonist efficacy and allosteric modulation
title_full_unstemmed The relationship between glycine receptor agonist efficacy and allosteric modulation
title_sort relationship between glycine receptor agonist efficacy and allosteric modulation
publishDate 2014
url http://hdl.handle.net/2152/24808
work_keys_str_mv AT kirsondean therelationshipbetweenglycinereceptoragonistefficacyandallostericmodulation
AT kirsondean relationshipbetweenglycinereceptoragonistefficacyandallostericmodulation
_version_ 1716823792209100800

Similar Items