Rapid Loss of Dendritic Spines after Stress Involves Derangement of Spine Dynamics by Corticotropin-Releasing Hormone

doi:10.1523/JNEUROSCI.0225-08.2008

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The Journal of Neuroscience, March 12, 2008, 28(11):2903-2911; doi:10.1523/JNEUROSCI.0225-08.2008

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Development/Plasticity/Repair
Rapid Loss of Dendritic Spines after Stress Involves Derangement of Spine Dynamics by Corticotropin-Releasing Hormone
Yuncai Chen,¹ Céline M. Dubé,¹ Courtney J. Rice,² and Tallie Z. Baram¹^,2
Departments of ¹Pediatrics and ²Anatomy/Neurobiology, University of California Irvine, Irvine, California 92697-4475
Correspondence should be addressed to Dr. Tallie Z. Baram, Departments of Pediatrics and Anatomy/Neurobiology, University of California Irvine, Medical Sciences I, ZOT: 4475, Irvine, CA 92697-4475. Email: tallie{at}uci.edu
Chronic stress causes dendritic regression and loss of dendriticspines in hippocampal neurons that is accompanied by deficitsin synaptic plasticity and memory. However, the responsiblemechanisms remain unresolved. Here, we found that within hoursof the onset of stress, the density of dendritic spines declinedin vulnerable dendritic domains. This rapid, stress-inducedspine loss was abolished by blocking the receptor (CRFR₁) ofcorticotropin-releasing hormone (CRH), a hippocampal neuropeptidereleased during stress. Exposure to CRH provoked spine lossand dendritic regression in hippocampal organotypic cultures,and selective blockade of the CRFR₁ receptor had the oppositeeffect. Live, time-lapse imaging revealed that CRH reduced spinedensity by altering dendritic spine dynamics: the peptide selectivelyand reversibly accelerated spine retraction, and this mechanisminvolved destabilization of spine F-actin. In addition, micelacking the CRFR₁ receptor had augmented spine density. Thesefindings support a mechanistic role for CRH–CRFR₁ signalingin stress-evoked spine loss and dendritic remodeling.

Key words: dendritic spine; stress; CRF; CRH; actin; synaptic plasticity; two photon; hippocampus

Received Nov. 21, 2007; accepted Feb. 4, 2008.

Correspondence should be addressed to Dr. Tallie Z. Baram, Departments of Pediatrics and Anatomy/Neurobiology, University of California Irvine, Medical Sciences I, ZOT: 4475, Irvine, CA 92697-4475. Email: tallie{at}uci.edu

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