Gephyrin regulates the cell surface dynamics of synaptic GABAA receptors
Gephyrin regulates the cell surface dynamics of synaptic GABAA receptors
The efficacy of fast synaptic inhibition is critically dependent on the accumulation of GABAA receptors at inhibitory synapses, a process that remains poorly understood. Here, we examined the dynamics of cell surface GABAA receptors using receptor subunits modified with N-terminal extracellular ecliptic pHluorin reporters. In hippocampal neurons, GABAA receptors incorporating pHluorin-tagged subunits were found to be clustered at synaptic sites and also expressed as diffuse extrasynaptic staining. By combining FRAP (fluorescence recovery after photobleaching) measurements with live imaging of FM4-64-labeled active presynaptic terminals, it was evident that clustered synaptic receptors exhibit significantly lower rates of mobility at the cell surface compared with their extrasynaptic counterparts. To examine the basis of this confinement, we used RNAi to inhibit the expression of gephyrin, a protein shown to regulate the accumulation of GABAA receptors at synaptic sites. However, whether gephyrin acts to control the actual formation of receptor clusters, their stability, or is simply a global regulator of receptor cell surface number remains unknown. Inhibiting gephyrin expression did not modify the total number of GABAA receptors expressed on the neuronal cell surface but significantly decreased the number of receptor clusters. Live imaging revealed that clusters that formed in the absence of gephyrin were significantly more mobile compared with those in control neurons. Together, our results demonstrate that synaptic GABAA receptors have lower levels of lateral mobility compared with their extrasynaptic counterparts, and suggest a specific role for gephyrin in reducing the diffusion of GABAA receptors, facilitating their accumulation at inhibitory synapses.
10469-10478
Jacob, TC
3e27d416-607d-4e30-b0af-4f8eb068eff4
Bogdanov, YD
0c970999-e191-4f1b-90d9-7bf25a5d5b4b
Magnus, C
08d16000-4760-49cc-b337-66833d2498b0
Saliba, RS
b3ee84be-6699-4ad5-95a8-fc2edd2975ec
Kittler, JT
ca98b44e-6463-4aee-9b39-b636f11bbd06
Haydon, PG
2c9f9351-7942-46cc-a341-aa484487ab03
Moss, SJ
b54ab8a8-a487-436c-9957-48a1382aaf2d
1 November 2005
Jacob, TC
3e27d416-607d-4e30-b0af-4f8eb068eff4
Bogdanov, YD
0c970999-e191-4f1b-90d9-7bf25a5d5b4b
Magnus, C
08d16000-4760-49cc-b337-66833d2498b0
Saliba, RS
b3ee84be-6699-4ad5-95a8-fc2edd2975ec
Kittler, JT
ca98b44e-6463-4aee-9b39-b636f11bbd06
Haydon, PG
2c9f9351-7942-46cc-a341-aa484487ab03
Moss, SJ
b54ab8a8-a487-436c-9957-48a1382aaf2d
Jacob, TC, Bogdanov, YD, Magnus, C, Saliba, RS, Kittler, JT, Haydon, PG and Moss, SJ
(2005)
Gephyrin regulates the cell surface dynamics of synaptic GABAA receptors.
Journal of Neuroscience, 25 (45), .
(doi:10.1523/jneurosci.2267-05.2005).
Abstract
The efficacy of fast synaptic inhibition is critically dependent on the accumulation of GABAA receptors at inhibitory synapses, a process that remains poorly understood. Here, we examined the dynamics of cell surface GABAA receptors using receptor subunits modified with N-terminal extracellular ecliptic pHluorin reporters. In hippocampal neurons, GABAA receptors incorporating pHluorin-tagged subunits were found to be clustered at synaptic sites and also expressed as diffuse extrasynaptic staining. By combining FRAP (fluorescence recovery after photobleaching) measurements with live imaging of FM4-64-labeled active presynaptic terminals, it was evident that clustered synaptic receptors exhibit significantly lower rates of mobility at the cell surface compared with their extrasynaptic counterparts. To examine the basis of this confinement, we used RNAi to inhibit the expression of gephyrin, a protein shown to regulate the accumulation of GABAA receptors at synaptic sites. However, whether gephyrin acts to control the actual formation of receptor clusters, their stability, or is simply a global regulator of receptor cell surface number remains unknown. Inhibiting gephyrin expression did not modify the total number of GABAA receptors expressed on the neuronal cell surface but significantly decreased the number of receptor clusters. Live imaging revealed that clusters that formed in the absence of gephyrin were significantly more mobile compared with those in control neurons. Together, our results demonstrate that synaptic GABAA receptors have lower levels of lateral mobility compared with their extrasynaptic counterparts, and suggest a specific role for gephyrin in reducing the diffusion of GABAA receptors, facilitating their accumulation at inhibitory synapses.
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Published date: 1 November 2005
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Copyright © 2005 Society for Neuroscience
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Local EPrints ID: 469801
URI: http://eprints.soton.ac.uk/id/eprint/469801
ISSN: 0270-6474
PURE UUID: 8c5f90e8-cf62-4dcc-ac2a-8646c2ea9776
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Date deposited: 26 Sep 2022 16:40
Last modified: 17 Mar 2024 03:37
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Author:
TC Jacob
Author:
C Magnus
Author:
RS Saliba
Author:
JT Kittler
Author:
PG Haydon
Author:
SJ Moss
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