GluR1 Links Structural and Functional Plasticity at Excitatory Synapses

doi:10.1523/JNEUROSCI.3503-07.2007

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The Journal of Neuroscience, December 12, 2007, 27(50):13706-13718; doi:10.1523/JNEUROSCI.3503-07.2007

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Cellular/Molecular
GluR1 Links Structural and Functional Plasticity at Excitatory Synapses
Charles D. Kopec,¹^,2 Eleonore Real,¹ Helmut W. Kessels,¹ and Roberto Malinow¹
¹Cold Spring Harbor Laboratory and ²Watson School of Biological Science, Cold Spring Harbor, New York 11724
Correspondence should be addressed to Roberto Malinow at the above address. Email: malinow{at}cshl.edu
Long-term potentiation (LTP), a cellular model of learning andmemory, produces both an enhancement of synaptic function andan increase in the size of the associated dendritic spine. Synapticinsertion of AMPA receptors is known to play an important rolein mediating the increase in synaptic strength during LTP, whereasthe role of AMPA receptor trafficking in structural changesremains unexplored. Here, we examine how the cell maintainsthe correlation between spine size and synapse strength duringLTP. We found that cells exploit an elegant solution by linkingboth processes to a single molecule: the AMPA-type glutamatereceptor subunit 1 (GluR1). Synaptic insertion of GluR1 is requiredto permit a stable increase in spine size, both in hippocampalslice cultures and in vivo. Synaptic insertion of GluR1 is notsufficient to drive structural plasticity. Although crucialto the expression of LTP, the ion channel function of GluR1is not required for the LTP-driven spine size enhancement. Remarkably,a recombinant cytosolic C-terminal fragment (C-tail) of GluR1is driven to the postsynaptic density after an LTP stimulus,and the synaptic incorporation of this isolated GluR1 C-tailis sufficient to permit spine enlargement even when postsynapticexocytosis of endogenous GluR1 is blocked. We conclude thatduring plasticity, synaptic insertion of GluR1 has two functions:the established role of increasing synaptic strength via itsligand-gated ion channel, and a novel role through the structurallystabilizing effect of its C terminus that permits an increasein spine size.

Key words: long-term potentiation; AMPA receptor; GluR1; spine; morphology; actin

Received Aug. 1, 2007; revised Oct. 19, 2007; accepted Oct. 23, 2007.

Correspondence should be addressed to Roberto Malinow at the above address. Email: malinow{at}cshl.edu

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