Allosteric interaction between the amino terminal domain and the ligand binding domain of NR2A

F. Zheng; K. Erreger; C. M. Low; T. Banke; C. J. Lee; P. J. Conn; S. F. Traynelis

doi:10.1038/nn0901-894

Allosteric interaction between the amino terminal domain and the ligand binding domain of NR2A

F. Zheng, K. Erreger, C. M. Low, T. Banke, C. J. Lee, P. J. Conn, S. F. Traynelis

KU-KIST Graduate School of Converging Science and Technology

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

54 Citations (Scopus)

Abstract

Fast desensitization is an important regulatory mechanism of neuronal NMDA receptor function. Only recombinant NMDA receptors composed of NR1/NR2A exhibit a fast component of desensitization similar to neuronal NMDA receptors. Here we report that the fast desensitization of NR1/NR2A receptors is caused by ambient zinc, and that a positive allosteric interaction occurs between the extracellular zinc-binding site located in the amino terminal domain and the glutamate-binding domain of NR2A. The relaxation of macroscopic currents reflects a shift to a new equilibrium due to increased zinc affinity after binding of glutamate. We also show a similar interaction between the ifenprodil binding site and the glutamate binding site of NR1/NR2B receptors. These data raise the possibility that there is an allosteric interaction between the amino terminal domain and the ligand-binding domain of other glutamate receptors. Our findings may provide insight into how zinc and other extracellular modulators regulate NMDA receptor function.

Original language	English
Pages (from-to)	894-901
Number of pages	8
Journal	Nature Neuroscience
Volume	4
Issue number	9
DOIs	https://doi.org/10.1038/nn0901-894
Publication status	Published - 2001

ASJC Scopus subject areas

Neuroscience(all)

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10.1038/nn0901-894

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@article{c605ef83ef564d76be0376fc7e5e29cc,

title = "Allosteric interaction between the amino terminal domain and the ligand binding domain of NR2A",

abstract = "Fast desensitization is an important regulatory mechanism of neuronal NMDA receptor function. Only recombinant NMDA receptors composed of NR1/NR2A exhibit a fast component of desensitization similar to neuronal NMDA receptors. Here we report that the fast desensitization of NR1/NR2A receptors is caused by ambient zinc, and that a positive allosteric interaction occurs between the extracellular zinc-binding site located in the amino terminal domain and the glutamate-binding domain of NR2A. The relaxation of macroscopic currents reflects a shift to a new equilibrium due to increased zinc affinity after binding of glutamate. We also show a similar interaction between the ifenprodil binding site and the glutamate binding site of NR1/NR2B receptors. These data raise the possibility that there is an allosteric interaction between the amino terminal domain and the ligand-binding domain of other glutamate receptors. Our findings may provide insight into how zinc and other extracellular modulators regulate NMDA receptor function.",

author = "F. Zheng and K. Erreger and Low, {C. M.} and T. Banke and Lee, {C. J.} and Conn, {P. J.} and Traynelis, {S. F.}",

note = "Funding Information: We thank M.L. Mayer, J. Neyton and P. Paoletti for reading the manuscript. S. F. Heinemann provided NR1 and NR2B. S. Nakanishi provided NR2A. D. Lynch and E. Aizenman provided NR2B(E201R). This work is supported by grants from NINDS (NS 39418 to F.Z., NS 36654 to S.F.T. and NS 31373 and NS 34876 to P.J. Conn), HHMI (K.E.), the Benzon Society (T.B.) and a Young Investigator Award from NARSAD to F.Z.",

year = "2001",

doi = "10.1038/nn0901-894",

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journal = "Nature Neuroscience",

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AU - Zheng, F.

AU - Erreger, K.

AU - Low, C. M.

AU - Banke, T.

AU - Lee, C. J.

AU - Conn, P. J.

AU - Traynelis, S. F.

N1 - Funding Information: We thank M.L. Mayer, J. Neyton and P. Paoletti for reading the manuscript. S. F. Heinemann provided NR1 and NR2B. S. Nakanishi provided NR2A. D. Lynch and E. Aizenman provided NR2B(E201R). This work is supported by grants from NINDS (NS 39418 to F.Z., NS 36654 to S.F.T. and NS 31373 and NS 34876 to P.J. Conn), HHMI (K.E.), the Benzon Society (T.B.) and a Young Investigator Award from NARSAD to F.Z.

PY - 2001

Y1 - 2001

N2 - Fast desensitization is an important regulatory mechanism of neuronal NMDA receptor function. Only recombinant NMDA receptors composed of NR1/NR2A exhibit a fast component of desensitization similar to neuronal NMDA receptors. Here we report that the fast desensitization of NR1/NR2A receptors is caused by ambient zinc, and that a positive allosteric interaction occurs between the extracellular zinc-binding site located in the amino terminal domain and the glutamate-binding domain of NR2A. The relaxation of macroscopic currents reflects a shift to a new equilibrium due to increased zinc affinity after binding of glutamate. We also show a similar interaction between the ifenprodil binding site and the glutamate binding site of NR1/NR2B receptors. These data raise the possibility that there is an allosteric interaction between the amino terminal domain and the ligand-binding domain of other glutamate receptors. Our findings may provide insight into how zinc and other extracellular modulators regulate NMDA receptor function.

AB - Fast desensitization is an important regulatory mechanism of neuronal NMDA receptor function. Only recombinant NMDA receptors composed of NR1/NR2A exhibit a fast component of desensitization similar to neuronal NMDA receptors. Here we report that the fast desensitization of NR1/NR2A receptors is caused by ambient zinc, and that a positive allosteric interaction occurs between the extracellular zinc-binding site located in the amino terminal domain and the glutamate-binding domain of NR2A. The relaxation of macroscopic currents reflects a shift to a new equilibrium due to increased zinc affinity after binding of glutamate. We also show a similar interaction between the ifenprodil binding site and the glutamate binding site of NR1/NR2B receptors. These data raise the possibility that there is an allosteric interaction between the amino terminal domain and the ligand-binding domain of other glutamate receptors. Our findings may provide insight into how zinc and other extracellular modulators regulate NMDA receptor function.

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Allosteric interaction between the amino terminal domain and the ligand binding domain of NR2A

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