Unraveling amino acid residues critical for allosteric potentiation of (α4)3(β2)2-type nicotinic acetylcholine receptor responses

Ze-Jun Wang; Farah Deba; Tasnim S Mohamed; David C Chiara; Kara Ramos; Ayman K Hamouda

doi:10.1074/jbc.M116.771246

Unraveling amino acid residues critical for allosteric potentiation of (α4)3(β2)2-type nicotinic acetylcholine receptor responses

J Biol Chem. 2017 Jun 16;292(24):9988-10001. doi: 10.1074/jbc.M116.771246. Epub 2017 Apr 26.

Authors

Ze-Jun Wang¹, Farah Deba¹, Tasnim S Mohamed¹, David C Chiara², Kara Ramos¹, Ayman K Hamouda^{3

4}

Affiliations

¹ From the Department of Pharmaceutical Sciences, Texas A&M Health Sciences Center, Kingsville, Texas 78363.
² Department of Neurobiology, Harvard Medical School, Boston, Massachusetts 02115.
³ From the Department of Pharmaceutical Sciences, Texas A&M Health Sciences Center, Kingsville, Texas 78363, Hamouda@tamhsc.edu.
⁴ Department of Neuroscience and Experimental Therapeutics, Texas A&M Health Sciences Center, Bryan, Texas 77807, and.

Abstract

Neuronal nicotinic acetylcholine receptors (nAChRs) are promising drug targets to manage several neurological disorders and nicotine addiction. Growing evidence indicates that positive allosteric modulators of nAChRs improve pharmacological specificity by binding to unique sites present only in a subpopulation of nAChRs. Furthermore, nAChR positive allosteric modulators such as NS9283 and CMPI have been shown to potentiate responses of (α4)3(β2)2 but not (α4)2(β2)3 nAChR isoforms. This selective potentiation underlines that the α4:α4 interface, which is present only in the (α4)3(β2)2 nAChR, is an important and promising drug target. In this report we used site-directed mutagenesis to substitute specific amino acid residues and computational analyses to elucidate CMPI's binding mode at the α4:α4 subunit extracellular interface and identified a unique set of amino acid residues that determined its affinity. We found that amino acid residues α4Gly-41, α4Lys-64, and α4Thr-66 were critical for (α4)3(β2)2 nAChR potentiation by CMPI, but not by NS9283, whereas amino acid substitution at α4His-116, a known determinant of NS9283 and of agonist binding at the α4:α4 subunit interface, did not reduce CMPI potentiation. In contrast, substitutions at α4Gln-124 and α4Thr-126 reduced potentiation by CMPI and NS9283, indicating that their binding sites partially overlap. These results delineate the role of amino acid residues contributing to the α4:α4 subunit extracellular interface in nAChR potentiation. These findings also provide structural information that will facilitate the structure-based design of novel therapeutics that target selectively the (α4)3(β2)2 nAChR.

Keywords: CMPI; NS9283; Positive allosteric modulators; dFBr; drug design; drug development; electrophysiology; ion channel; nicotinic acetylcholine receptors (nAChR); pentameric ligand-gated ion channel.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Amino Acid Substitution
Animals
Humans
Hydrocarbons, Brominated / chemistry
Hydrocarbons, Brominated / metabolism
Hydrocarbons, Brominated / pharmacology
Indole Alkaloids / chemistry
Indole Alkaloids / metabolism
Indole Alkaloids / pharmacology
Isoxazoles / chemistry
Isoxazoles / metabolism
Isoxazoles / pharmacology
Ligands
Models, Molecular*
Molecular Docking Simulation
Nerve Tissue Proteins / agonists
Nerve Tissue Proteins / chemistry
Nerve Tissue Proteins / genetics
Nerve Tissue Proteins / metabolism*
Nicotinic Agonists / chemistry
Nicotinic Agonists / metabolism*
Nicotinic Agonists / pharmacology
Oocytes / drug effects
Oocytes / metabolism
Oxadiazoles / chemistry
Oxadiazoles / metabolism
Oxadiazoles / pharmacology
Patch-Clamp Techniques
Point Mutation
Protein Conformation
Protein Interaction Domains and Motifs
Pyrazoles / chemistry
Pyrazoles / metabolism
Pyrazoles / pharmacology
Pyridines / chemistry
Pyridines / metabolism
Pyridines / pharmacology
Receptors, Nicotinic / chemistry
Receptors, Nicotinic / genetics
Receptors, Nicotinic / metabolism*
Recombinant Proteins / chemistry
Recombinant Proteins / metabolism
Structural Homology, Protein
Xenopus laevis

Substances

3-(2-chlorophenyl)-5-(5-methyl-1-(piperidin-4-yl)-1H-pyrazol-4-yl)isoxazole
3-(3-(pyridine-3-yl)-1,2,4-oxadiazol-5-yl)benzonitrile
Hydrocarbons, Brominated
Indole Alkaloids
Isoxazoles
Ligands
Nerve Tissue Proteins
Nicotinic Agonists
Oxadiazoles
Pyrazoles
Pyridines
Receptors, Nicotinic
Recombinant Proteins
desformylflustrabromine
nicotinic acetylcholine receptor alpha4 subunit
nicotinic receptor alpha4beta2
nicotinic receptor beta2

Associated data

PDB/5KXI
PDB/1UV6
PDB/5KXI.PDB

Grants and funding

R15 NS093590/NS/NINDS NIH HHS/United States