Structural basis of long-term potentiation in single dendritic spines

被引:0
作者
Masanori Matsuzaki
Naoki Honkura
Graham C. R. Ellis-Davies
Haruo Kasai
机构
[1] National Institute for Physiological Sciences and The Graduate University of Advanced Studies (Sokendai),Department of Cell Physiology
[2] Drexel University College of Medicine,Department of Pharmacology and Physiology
来源
Nature | 2004年 / 429卷
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摘要
Dendritic spines of pyramidal neurons in the cerebral cortex undergo activity-dependent structural remodelling1,2,3,4,5 that has been proposed to be a cellular basis of learning and memory6. How structural remodelling supports synaptic plasticity4,5, such as long-term potentiation7, and whether such plasticity is input-specific at the level of the individual spine has remained unknown. We investigated the structural basis of long-term potentiation using two-photon photolysis of caged glutamate at single spines of hippocampal CA1 pyramidal neurons8. Here we show that repetitive quantum-like photorelease (uncaging) of glutamate induces a rapid and selective enlargement of stimulated spines that is transient in large mushroom spines but persistent in small spines. Spine enlargement is associated with an increase in AMPA-receptor-mediated currents at the stimulated synapse and is dependent on NMDA receptors, calmodulin and actin polymerization. Long-lasting spine enlargement also requires Ca2+/calmodulin-dependent protein kinase II. Our results thus indicate that spines individually follow Hebb's postulate for learning. They further suggest that small spines are preferential sites for long-term potentiation induction, whereas large spines might represent physical traces of long-term memory.
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页码:761 / 766
页数:5
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