Pharmacological and structural characterization of conformationally restricted (S)-glutamate analogues at ionotropic glutamate receptors

Lina Juknaite; Raminta Venskutonyte; Zeinab Assaf; Sophie Faure; Thierry Gefflaut; David J. Aitken; Birgitte Nielsen; Michael Gajhede; Jette Sandholm Jensen Kastrup; Lennart Bunch; Karla Frydenvang; Darryl S. Pickering

doi:10.1016/j.jsb.2012.07.001

Pharmacological and structural characterization of conformationally restricted (S)-glutamate analogues at ionotropic glutamate receptors

Lina Juknaite, Raminta Venskutonyte, Zeinab Assaf, Sophie Faure, Thierry Gefflaut, David J. Aitken, Birgitte Nielsen, Michael Gajhede, Jette Sandholm Jensen Kastrup, Lennart Bunch, Karla Frydenvang, Darryl S. Pickering

9 Citationer (Scopus)

Abstract

Conformationally restricted glutamate analogues have been pharmacologically characterized at AMPA and kainate receptors and the crystal structures have been solved of the ligand (2S,1'R,2'S)-2-(2'-carboxycyclobutyl)glycine (CBG-IV) in complex with the ligand binding domains of the AMPA receptor GluA2 and the kainate receptor GluK3. These structures show that CBG-IV interacts with the binding pocket in the same way as (S)-glutamate. The binding affinities reveal that CBG-IV has high affinity at the AMPA and kainate receptor subtypes. Appreciable binding affinity of CBG-IV was not observed at NMDA receptors, where the introduction of the carbocyclic ring is expected to lead to a steric clash with binding site residues. CBG-IV was demonstrated to be an agonist at both GluA2 and the kainate receptor GluK1. CBG-IV showed high affinity binding to GluK1 compared to GluA2, GluK2 and GluK3, which exhibited lower affinity for CBG-IV. The structure of GluA2 LBD and GluK3 LBD in complex with CBG-IV revealed similar binding site interactions to those of (S)-glutamate. No major conformational rearrangements compared to the (S)-glutamate bound conformation were found in GluK3 in order to accommodate CBG-IV, in contrast with GluA2 where a shift in lobe D2 binding site residues occurs, leading to an increased binding cavity volume compared to the (S)-glutamate bound structure.

Originalsprog	Engelsk
Tidsskrift	Journal of Structural Biology
Vol/bind	180
Udgave nummer	1
Sider (fra-til)	39-46
ISSN	1047-8477
DOI	https://doi.org/10.1016/j.jsb.2012.07.001
Status	Udgivet - okt. 2012

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10.1016/j.jsb.2012.07.001

Citationsformater

Juknaite, L., Venskutonyte, R., Assaf, Z., Faure, S., Gefflaut, T., Aitken, D. J., Nielsen, B., Gajhede, M., Kastrup, J. S. J., Bunch, L., Frydenvang, K., & Pickering, D. S. (2012). Pharmacological and structural characterization of conformationally restricted (S)-glutamate analogues at ionotropic glutamate receptors. Journal of Structural Biology, 180(1), 39-46. https://doi.org/10.1016/j.jsb.2012.07.001

Juknaite, L, Venskutonyte, R, Assaf, Z, Faure, S, Gefflaut, T, Aitken, DJ, Nielsen, B , Gajhede, M , Kastrup, JSJ , Bunch, L , Frydenvang, K & Pickering, DS 2012, 'Pharmacological and structural characterization of conformationally restricted (S)-glutamate analogues at ionotropic glutamate receptors', Journal of Structural Biology, bind 180, nr. 1, s. 39-46. https://doi.org/10.1016/j.jsb.2012.07.001

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title = "Pharmacological and structural characterization of conformationally restricted (S)-glutamate analogues at ionotropic glutamate receptors",

abstract = "Conformationally restricted glutamate analogues have been pharmacologically characterized at AMPA and kainate receptors and the crystal structures have been solved of the ligand (2S,1'R,2'S)-2-(2'-carboxycyclobutyl)glycine (CBG-IV) in complex with the ligand binding domains of the AMPA receptor GluA2 and the kainate receptor GluK3. These structures show that CBG-IV interacts with the binding pocket in the same way as (S)-glutamate. The binding affinities reveal that CBG-IV has high affinity at the AMPA and kainate receptor subtypes. Appreciable binding affinity of CBG-IV was not observed at NMDA receptors, where the introduction of the carbocyclic ring is expected to lead to a steric clash with binding site residues. CBG-IV was demonstrated to be an agonist at both GluA2 and the kainate receptor GluK1. CBG-IV showed high affinity binding to GluK1 compared to GluA2, GluK2 and GluK3, which exhibited lower affinity for CBG-IV. The structure of GluA2 LBD and GluK3 LBD in complex with CBG-IV revealed similar binding site interactions to those of (S)-glutamate. No major conformational rearrangements compared to the (S)-glutamate bound conformation were found in GluK3 in order to accommodate CBG-IV, in contrast with GluA2 where a shift in lobe D2 binding site residues occurs, leading to an increased binding cavity volume compared to the (S)-glutamate bound structure.",

author = "Lina Juknaite and Raminta Venskutonyte and Zeinab Assaf and Sophie Faure and Thierry Gefflaut and Aitken, {David J.} and Birgitte Nielsen and Michael Gajhede and Kastrup, {Jette Sandholm Jensen} and Lennart Bunch and Karla Frydenvang and Pickering, {Darryl S.}",

note = "Copyright {\textcopyright} 2012. Published by Elsevier Inc.",

year = "2012",

month = oct,

doi = "10.1016/j.jsb.2012.07.001",

language = "English",

volume = "180",

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T1 - Pharmacological and structural characterization of conformationally restricted (S)-glutamate analogues at ionotropic glutamate receptors

AU - Juknaite, Lina

AU - Venskutonyte, Raminta

AU - Assaf, Zeinab

AU - Faure, Sophie

AU - Gefflaut, Thierry

AU - Aitken, David J.

AU - Nielsen, Birgitte

AU - Gajhede, Michael

AU - Kastrup, Jette Sandholm Jensen

AU - Bunch, Lennart

AU - Frydenvang, Karla

AU - Pickering, Darryl S.

PY - 2012/10

Y1 - 2012/10

N2 - Conformationally restricted glutamate analogues have been pharmacologically characterized at AMPA and kainate receptors and the crystal structures have been solved of the ligand (2S,1'R,2'S)-2-(2'-carboxycyclobutyl)glycine (CBG-IV) in complex with the ligand binding domains of the AMPA receptor GluA2 and the kainate receptor GluK3. These structures show that CBG-IV interacts with the binding pocket in the same way as (S)-glutamate. The binding affinities reveal that CBG-IV has high affinity at the AMPA and kainate receptor subtypes. Appreciable binding affinity of CBG-IV was not observed at NMDA receptors, where the introduction of the carbocyclic ring is expected to lead to a steric clash with binding site residues. CBG-IV was demonstrated to be an agonist at both GluA2 and the kainate receptor GluK1. CBG-IV showed high affinity binding to GluK1 compared to GluA2, GluK2 and GluK3, which exhibited lower affinity for CBG-IV. The structure of GluA2 LBD and GluK3 LBD in complex with CBG-IV revealed similar binding site interactions to those of (S)-glutamate. No major conformational rearrangements compared to the (S)-glutamate bound conformation were found in GluK3 in order to accommodate CBG-IV, in contrast with GluA2 where a shift in lobe D2 binding site residues occurs, leading to an increased binding cavity volume compared to the (S)-glutamate bound structure.

AB - Conformationally restricted glutamate analogues have been pharmacologically characterized at AMPA and kainate receptors and the crystal structures have been solved of the ligand (2S,1'R,2'S)-2-(2'-carboxycyclobutyl)glycine (CBG-IV) in complex with the ligand binding domains of the AMPA receptor GluA2 and the kainate receptor GluK3. These structures show that CBG-IV interacts with the binding pocket in the same way as (S)-glutamate. The binding affinities reveal that CBG-IV has high affinity at the AMPA and kainate receptor subtypes. Appreciable binding affinity of CBG-IV was not observed at NMDA receptors, where the introduction of the carbocyclic ring is expected to lead to a steric clash with binding site residues. CBG-IV was demonstrated to be an agonist at both GluA2 and the kainate receptor GluK1. CBG-IV showed high affinity binding to GluK1 compared to GluA2, GluK2 and GluK3, which exhibited lower affinity for CBG-IV. The structure of GluA2 LBD and GluK3 LBD in complex with CBG-IV revealed similar binding site interactions to those of (S)-glutamate. No major conformational rearrangements compared to the (S)-glutamate bound conformation were found in GluK3 in order to accommodate CBG-IV, in contrast with GluA2 where a shift in lobe D2 binding site residues occurs, leading to an increased binding cavity volume compared to the (S)-glutamate bound structure.

U2 - 10.1016/j.jsb.2012.07.001

DO - 10.1016/j.jsb.2012.07.001

M3 - Journal article

C2 - 22789682

SN - 1047-8477

VL - 180

SP - 39

EP - 46

JO - Journal of Structural Biology

JF - Journal of Structural Biology

IS - 1

ER -

Pharmacological and structural characterization of conformationally restricted (S)-glutamate analogues at ionotropic glutamate receptors

Abstract

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