Plasmon-waveguide resonance spectroscopy: A new tool for investigating signal transduction by G-protein coupled receptors

Gordon Tollin; Zdzislaw Salamon; Scott Cowell; Victor J. Hruby

doi:10.1016/j.lfs.2003.07.001

Plasmon-waveguide resonance spectroscopy: A new tool for investigating signal transduction by G-protein coupled receptors

Gordon Tollin, Zdzislaw Salamon, Scott Cowell, Victor J. Hruby

Chemistry and Biochemistry

Research output: Contribution to journal › Article › peer-review

7 Scopus citations

Abstract

Plasmon-waveguide resonance (PWR) spectroscopy provides a highly sensitive method for characterizing the kinetics, affinities and conformational changes involved in ligand binding to G-protein coupled receptors, without the need for radioactive or other labeling strategies. In the case of the cloned δ-opioid receptor from human brain incorporated into a lipid bilayer, we have shown that affinities determined in this way are consistent with those measured by standard binding procedures using membranes or whole cells containing the receptors, and that the spectral and kinetic properties of the binding processes allow facile distinction between agonist, inverse agonist, and antagonist ligands. We have also shown by direct measurements that G-protein binding affinities and the ability to undergo GTP/GDP exchange are dependent upon the type of ligand pre-bound to the receptor. PWR spectroscopy thus provides a powerful new approach to investigating signal transduction in biological membrane systems.

Original language	English (US)
Pages (from-to)	3307-3311
Number of pages	5
Journal	Life Sciences
Volume	73
Issue number	26
DOIs	https://doi.org/10.1016/j.lfs.2003.07.001
State	Published - Nov 14 2003

Keywords

Human delta-opioid receptor
Ligand binding
Lipid bilayers
Plasmon-waveguide resonance spectroscopy
Receptor conformational states

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology
Pharmacology, Toxicology and Pharmaceutics(all)

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10.1016/j.lfs.2003.07.001

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title = "Plasmon-waveguide resonance spectroscopy: A new tool for investigating signal transduction by G-protein coupled receptors",

abstract = "Plasmon-waveguide resonance (PWR) spectroscopy provides a highly sensitive method for characterizing the kinetics, affinities and conformational changes involved in ligand binding to G-protein coupled receptors, without the need for radioactive or other labeling strategies. In the case of the cloned δ-opioid receptor from human brain incorporated into a lipid bilayer, we have shown that affinities determined in this way are consistent with those measured by standard binding procedures using membranes or whole cells containing the receptors, and that the spectral and kinetic properties of the binding processes allow facile distinction between agonist, inverse agonist, and antagonist ligands. We have also shown by direct measurements that G-protein binding affinities and the ability to undergo GTP/GDP exchange are dependent upon the type of ligand pre-bound to the receptor. PWR spectroscopy thus provides a powerful new approach to investigating signal transduction in biological membrane systems.",

keywords = "Human delta-opioid receptor, Ligand binding, Lipid bilayers, Plasmon-waveguide resonance spectroscopy, Receptor conformational states",

author = "Gordon Tollin and Zdzislaw Salamon and Scott Cowell and Hruby, {Victor J.}",

note = "Funding Information: This work was supported in part by grants from the National Science Foundation (MCB-9904753 to G.T. and Z.S.), the National Institutes of Health (GM59630 to G.T. and Z.S.), and the National Institute of Drug Abuse (DA-06284 and DA-13449 to V.J.H.), and a U.S. Public Health Service Postdoctoral Fellowship (DA-05787 to S.C.).",

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AU - Salamon, Zdzislaw

AU - Cowell, Scott

AU - Hruby, Victor J.

N1 - Funding Information: This work was supported in part by grants from the National Science Foundation (MCB-9904753 to G.T. and Z.S.), the National Institutes of Health (GM59630 to G.T. and Z.S.), and the National Institute of Drug Abuse (DA-06284 and DA-13449 to V.J.H.), and a U.S. Public Health Service Postdoctoral Fellowship (DA-05787 to S.C.).

PY - 2003/11/14

Y1 - 2003/11/14

N2 - Plasmon-waveguide resonance (PWR) spectroscopy provides a highly sensitive method for characterizing the kinetics, affinities and conformational changes involved in ligand binding to G-protein coupled receptors, without the need for radioactive or other labeling strategies. In the case of the cloned δ-opioid receptor from human brain incorporated into a lipid bilayer, we have shown that affinities determined in this way are consistent with those measured by standard binding procedures using membranes or whole cells containing the receptors, and that the spectral and kinetic properties of the binding processes allow facile distinction between agonist, inverse agonist, and antagonist ligands. We have also shown by direct measurements that G-protein binding affinities and the ability to undergo GTP/GDP exchange are dependent upon the type of ligand pre-bound to the receptor. PWR spectroscopy thus provides a powerful new approach to investigating signal transduction in biological membrane systems.

AB - Plasmon-waveguide resonance (PWR) spectroscopy provides a highly sensitive method for characterizing the kinetics, affinities and conformational changes involved in ligand binding to G-protein coupled receptors, without the need for radioactive or other labeling strategies. In the case of the cloned δ-opioid receptor from human brain incorporated into a lipid bilayer, we have shown that affinities determined in this way are consistent with those measured by standard binding procedures using membranes or whole cells containing the receptors, and that the spectral and kinetic properties of the binding processes allow facile distinction between agonist, inverse agonist, and antagonist ligands. We have also shown by direct measurements that G-protein binding affinities and the ability to undergo GTP/GDP exchange are dependent upon the type of ligand pre-bound to the receptor. PWR spectroscopy thus provides a powerful new approach to investigating signal transduction in biological membrane systems.

KW - Human delta-opioid receptor

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KW - Plasmon-waveguide resonance spectroscopy

KW - Receptor conformational states

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Plasmon-waveguide resonance spectroscopy: A new tool for investigating signal transduction by G-protein coupled receptors

Abstract

Keywords

ASJC Scopus subject areas

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