[PDF][PDF] Subunit composition of synaptic AMPA receptors revealed by a single-cell genetic approach

W Lu, Y Shi, AC Jackson, K Bjorgan, MJ During… - Neuron, 2009 - cell.com
W Lu, Y Shi, AC Jackson, K Bjorgan, MJ During, R Sprengel, PH Seeburg, RA Nicoll
Neuron, 2009cell.com
The precise subunit composition of synaptic ionotropic receptors in the brain is poorly
understood. This information is of particular importance with regard to AMPA-type glutamate
receptors, the multimeric complexes assembled from GluA1-A4 subunits, as the trafficking of
these receptors into and out of synapses is proposed to depend upon the subunit
composition of the receptor. We report a molecular quantification of synaptic AMPA
receptors (AMPARs) by employing a single-cell genetic approach coupled with …
Summary
The precise subunit composition of synaptic ionotropic receptors in the brain is poorly understood. This information is of particular importance with regard to AMPA-type glutamate receptors, the multimeric complexes assembled from GluA1-A4 subunits, as the trafficking of these receptors into and out of synapses is proposed to depend upon the subunit composition of the receptor. We report a molecular quantification of synaptic AMPA receptors (AMPARs) by employing a single-cell genetic approach coupled with electrophysiology in hippocampal CA1 pyramidal neurons. In contrast to prevailing views, we find that GluA1A2 heteromers are the dominant AMPARs at CA1 cell synapses (∼80%). In cells lacking GluA1, -A2, and -A3, synapses are devoid of AMPARs, yet synaptic NMDA receptors (NMDARs) and dendritic morphology remain unchanged. These data demonstrate a functional dissociation of AMPARs from trafficking of NMDARs and neuronal morphogenesis. This study provides a functional quantification of the subunit composition of AMPARs in the CNS and suggests novel roles for AMPAR subunits in receptor trafficking.
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