Engineered α4β2 nicotinic acetylcholine receptors as models for measuring agonist binding and effect at the orthosteric low-affinity α4-α4 interface

Philip K. Ahring; Jeppe A. Olsen; Elsebet O. Nielsen; Dan Peters; Martin Holst Friborg Pedersen; Line A. Rohde; Jette S. Kastrup; Azadeh Shahsavar; Dinesh C. Indurthi; Mary Chebib; Michael Gajhede; Thomas Balle

doi:10.1016/j.neuropharm.2014.12.035

Engineered α4β2 nicotinic acetylcholine receptors as models for measuring agonist binding and effect at the orthosteric low-affinity α4-α4 interface

Philip K. Ahring, Jeppe A. Olsen, Elsebet O. Nielsen, Dan Peters, Martin Holst Friborg Pedersen, Line A. Rohde, Jette S. Kastrup, Azadeh Shahsavar, Dinesh C. Indurthi, Mary Chebib, Michael Gajhede, Thomas Balle

Research output: Contribution to journal › Journal article › Research › peer-review

Abstract

The nicotinic acetylcholine receptor alpha 4 beta 2 is important for normal mammalian brain function and is known to express in two different stoichiometries, (alpha 4)(2)(beta 2)(3) and (alpha 4)(3)(beta 2)(2). While these are similar in many aspects, the (alpha 4)(3)(beta 2)(2) stoichiometry differs by harboring a third orthosteric acetylcholine binding site located at the alpha 4-alpha 4 interface. Interestingly, the third binding site has, so far, only been documented using electrophysiological assays, actual binding affinities of nicotinic receptor ligands to this site are not known. The present study was therefore aimed at determining binding affinities of nicotinic ligands to the alpha 4-alpha 4 interface. Given that epibatidine shows large functional potency differences at alpha 4-beta 2 vs. alpha 4-alpha 4 interfaces, biphasic binding properties would be expected at (alpha 4)(3)(beta 2)(2) receptors. However, standard saturation binding experiments with [H-3]epibatidine did not reveal biphasic binding under the conditions utilized. Therefore, an engineered beta 2 construct (beta 2(HQT)), which converts the beta(-) face to resemble that of an alpha 4(-) face, was utilized to create (alpha 4)(3)(beta 2(HQT))(2) receptors harboring three alpha 4-alpha 4 interfaces. With this receptor, low affinity binding of epibatidine with a K-d of similar to 5 nM was observed in sharp contrast to a K-d value of similar to 10 pM observed for wild-type receptors. A strong correlation between binding affinities at the (alpha 4)(3)(beta 2(HQT))(2) receptor and functional potencies at the wild-type receptor of a range of nicotinic ligands highlighted the validity of using the mutational approach. Finally, large differences in activities at alpha 4-beta 2 vs. alpha 4-alpha 4 interfaces were observed for structurally related agonists underscoring the need for establishing all binding parameters of compounds at alpha 4 beta 2 receptors. Crown Copyright (C) 2015 Published by Elsevier Ltd. All rights reserved.

Original language	English
Journal	Neuropharmacology
Volume	92
Pages (from-to)	135-145
Number of pages	11
ISSN	0028-3908
DOIs	https://doi.org/10.1016/j.neuropharm.2014.12.035
Publication status	Published - 2015

Keywords

NEUROSCIENCES
PHARMACOLOGY
POSITIVE ALLOSTERIC MODULATOR
ALTERNATE STOICHIOMETRIES
CHOLINERGIC-RECEPTORS
EPIBATIDINE BINDING
LOW-SENSITIVITY
NATIVE BRAIN
DOUBLE-BLIND
IN-VIVO
EFFICACY
NS9283
Cys-loop receptor
Nicotinic acetylcholine receptor (nAChR)
Ion channel
Pharmacology
Electrophysiology
Radioligand binding

Access to Document

10.1016/j.neuropharm.2014.12.035

OpenUrl availability

Full text

Cite this

Ahring, P. K., Olsen, J. A., Nielsen, E. O., Peters, D., Pedersen, M. H. F., Rohde, L. A., Kastrup, J. S., Shahsavar, A., Indurthi, D. C., Chebib, M., Gajhede, M., & Balle, T. (2015). Engineered α4β2 nicotinic acetylcholine receptors as models for measuring agonist binding and effect at the orthosteric low-affinity α4-α4 interface. Neuropharmacology, 92, 135-145. https://doi.org/10.1016/j.neuropharm.2014.12.035

@article{1e9029b92dcc42ba9aff3287c01fbf35,

title = "Engineered α4β2 nicotinic acetylcholine receptors as models for measuring agonist binding and effect at the orthosteric low-affinity α4-α4 interface",

abstract = "The nicotinic acetylcholine receptor alpha 4 beta 2 is important for normal mammalian brain function and is known to express in two different stoichiometries, (alpha 4)(2)(beta 2)(3) and (alpha 4)(3)(beta 2)(2). While these are similar in many aspects, the (alpha 4)(3)(beta 2)(2) stoichiometry differs by harboring a third orthosteric acetylcholine binding site located at the alpha 4-alpha 4 interface. Interestingly, the third binding site has, so far, only been documented using electrophysiological assays, actual binding affinities of nicotinic receptor ligands to this site are not known. The present study was therefore aimed at determining binding affinities of nicotinic ligands to the alpha 4-alpha 4 interface. Given that epibatidine shows large functional potency differences at alpha 4-beta 2 vs. alpha 4-alpha 4 interfaces, biphasic binding properties would be expected at (alpha 4)(3)(beta 2)(2) receptors. However, standard saturation binding experiments with [H-3]epibatidine did not reveal biphasic binding under the conditions utilized. Therefore, an engineered beta 2 construct (beta 2(HQT)), which converts the beta(-) face to resemble that of an alpha 4(-) face, was utilized to create (alpha 4)(3)(beta 2(HQT))(2) receptors harboring three alpha 4-alpha 4 interfaces. With this receptor, low affinity binding of epibatidine with a K-d of similar to 5 nM was observed in sharp contrast to a K-d value of similar to 10 pM observed for wild-type receptors. A strong correlation between binding affinities at the (alpha 4)(3)(beta 2(HQT))(2) receptor and functional potencies at the wild-type receptor of a range of nicotinic ligands highlighted the validity of using the mutational approach. Finally, large differences in activities at alpha 4-beta 2 vs. alpha 4-alpha 4 interfaces were observed for structurally related agonists underscoring the need for establishing all binding parameters of compounds at alpha 4 beta 2 receptors. Crown Copyright (C) 2015 Published by Elsevier Ltd. All rights reserved.",

keywords = "NEUROSCIENCES, PHARMACOLOGY, POSITIVE ALLOSTERIC MODULATOR, ALTERNATE STOICHIOMETRIES, CHOLINERGIC-RECEPTORS, EPIBATIDINE BINDING, LOW-SENSITIVITY, NATIVE BRAIN, DOUBLE-BLIND, IN-VIVO, EFFICACY, NS9283, Cys-loop receptor, Nicotinic acetylcholine receptor (nAChR), Ion channel, Pharmacology, Electrophysiology, Radioligand binding",

author = "Ahring, {Philip K.} and Olsen, {Jeppe A.} and Nielsen, {Elsebet O.} and Dan Peters and Pedersen, {Martin Holst Friborg} and Rohde, {Line A.} and Kastrup, {Jette S.} and Azadeh Shahsavar and Indurthi, {Dinesh C.} and Mary Chebib and Michael Gajhede and Thomas Balle",

year = "2015",

doi = "10.1016/j.neuropharm.2014.12.035",

language = "English",

volume = "92",

pages = "135--145",

journal = "Neuropharmacology",

issn = "0028-3908",

publisher = "Pergamon Press",

}

Ahring, PK, Olsen, JA, Nielsen, EO, Peters, D, Pedersen, MHF, Rohde, LA, Kastrup, JS, Shahsavar, A, Indurthi, DC, Chebib, M, Gajhede, M & Balle, T 2015, 'Engineered α4β2 nicotinic acetylcholine receptors as models for measuring agonist binding and effect at the orthosteric low-affinity α4-α4 interface', Neuropharmacology, vol. 92, pp. 135-145. https://doi.org/10.1016/j.neuropharm.2014.12.035

TY - JOUR

T1 - Engineered α4β2 nicotinic acetylcholine receptors as models for measuring agonist binding and effect at the orthosteric low-affinity α4-α4 interface

AU - Ahring, Philip K.

AU - Olsen, Jeppe A.

AU - Nielsen, Elsebet O.

AU - Peters, Dan

AU - Pedersen, Martin Holst Friborg

AU - Rohde, Line A.

AU - Kastrup, Jette S.

AU - Shahsavar, Azadeh

AU - Indurthi, Dinesh C.

AU - Chebib, Mary

AU - Gajhede, Michael

AU - Balle, Thomas

PY - 2015

Y1 - 2015

N2 - The nicotinic acetylcholine receptor alpha 4 beta 2 is important for normal mammalian brain function and is known to express in two different stoichiometries, (alpha 4)(2)(beta 2)(3) and (alpha 4)(3)(beta 2)(2). While these are similar in many aspects, the (alpha 4)(3)(beta 2)(2) stoichiometry differs by harboring a third orthosteric acetylcholine binding site located at the alpha 4-alpha 4 interface. Interestingly, the third binding site has, so far, only been documented using electrophysiological assays, actual binding affinities of nicotinic receptor ligands to this site are not known. The present study was therefore aimed at determining binding affinities of nicotinic ligands to the alpha 4-alpha 4 interface. Given that epibatidine shows large functional potency differences at alpha 4-beta 2 vs. alpha 4-alpha 4 interfaces, biphasic binding properties would be expected at (alpha 4)(3)(beta 2)(2) receptors. However, standard saturation binding experiments with [H-3]epibatidine did not reveal biphasic binding under the conditions utilized. Therefore, an engineered beta 2 construct (beta 2(HQT)), which converts the beta(-) face to resemble that of an alpha 4(-) face, was utilized to create (alpha 4)(3)(beta 2(HQT))(2) receptors harboring three alpha 4-alpha 4 interfaces. With this receptor, low affinity binding of epibatidine with a K-d of similar to 5 nM was observed in sharp contrast to a K-d value of similar to 10 pM observed for wild-type receptors. A strong correlation between binding affinities at the (alpha 4)(3)(beta 2(HQT))(2) receptor and functional potencies at the wild-type receptor of a range of nicotinic ligands highlighted the validity of using the mutational approach. Finally, large differences in activities at alpha 4-beta 2 vs. alpha 4-alpha 4 interfaces were observed for structurally related agonists underscoring the need for establishing all binding parameters of compounds at alpha 4 beta 2 receptors. Crown Copyright (C) 2015 Published by Elsevier Ltd. All rights reserved.

AB - The nicotinic acetylcholine receptor alpha 4 beta 2 is important for normal mammalian brain function and is known to express in two different stoichiometries, (alpha 4)(2)(beta 2)(3) and (alpha 4)(3)(beta 2)(2). While these are similar in many aspects, the (alpha 4)(3)(beta 2)(2) stoichiometry differs by harboring a third orthosteric acetylcholine binding site located at the alpha 4-alpha 4 interface. Interestingly, the third binding site has, so far, only been documented using electrophysiological assays, actual binding affinities of nicotinic receptor ligands to this site are not known. The present study was therefore aimed at determining binding affinities of nicotinic ligands to the alpha 4-alpha 4 interface. Given that epibatidine shows large functional potency differences at alpha 4-beta 2 vs. alpha 4-alpha 4 interfaces, biphasic binding properties would be expected at (alpha 4)(3)(beta 2)(2) receptors. However, standard saturation binding experiments with [H-3]epibatidine did not reveal biphasic binding under the conditions utilized. Therefore, an engineered beta 2 construct (beta 2(HQT)), which converts the beta(-) face to resemble that of an alpha 4(-) face, was utilized to create (alpha 4)(3)(beta 2(HQT))(2) receptors harboring three alpha 4-alpha 4 interfaces. With this receptor, low affinity binding of epibatidine with a K-d of similar to 5 nM was observed in sharp contrast to a K-d value of similar to 10 pM observed for wild-type receptors. A strong correlation between binding affinities at the (alpha 4)(3)(beta 2(HQT))(2) receptor and functional potencies at the wild-type receptor of a range of nicotinic ligands highlighted the validity of using the mutational approach. Finally, large differences in activities at alpha 4-beta 2 vs. alpha 4-alpha 4 interfaces were observed for structurally related agonists underscoring the need for establishing all binding parameters of compounds at alpha 4 beta 2 receptors. Crown Copyright (C) 2015 Published by Elsevier Ltd. All rights reserved.

KW - NEUROSCIENCES

KW - PHARMACOLOGY

KW - POSITIVE ALLOSTERIC MODULATOR

KW - ALTERNATE STOICHIOMETRIES

KW - CHOLINERGIC-RECEPTORS

KW - EPIBATIDINE BINDING

KW - LOW-SENSITIVITY

KW - NATIVE BRAIN

KW - DOUBLE-BLIND

KW - IN-VIVO

KW - EFFICACY

KW - NS9283

KW - Cys-loop receptor

KW - Nicotinic acetylcholine receptor (nAChR)

KW - Ion channel

KW - Pharmacology

KW - Electrophysiology

KW - Radioligand binding

U2 - 10.1016/j.neuropharm.2014.12.035

DO - 10.1016/j.neuropharm.2014.12.035

M3 - Journal article

C2 - 25595102

SN - 0028-3908

VL - 92

SP - 135

EP - 145

JO - Neuropharmacology

JF - Neuropharmacology

ER -

Engineered α4β2 nicotinic acetylcholine receptors as models for measuring agonist binding and effect at the orthosteric low-affinity α4-α4 interface

Abstract

Keywords

Access to Document

OpenUrl availability

Fingerprint

Cite this