Your search keyword '"George W. Huntley"' showing total 3 results

1. N-cadherin regulates molecular organization of excitatory and inhibitory synaptic circuits in adult hippocampus in vivo

Author

Matthew L. Shapiro, Shekhar B. Patil, Deanna L. Benson, Jessica S. Nikitczuk, George W. Huntley, Joseph R. Scarpa, and Bridget A. Matikainen-Ankney

Subjects

Synapse, Synaptic pharmacology, Cognitive Neuroscience, Silent synapse, Metaplasticity, Synaptic plasticity, Biological neural network, Biology, Inhibitory postsynaptic potential, Neuroscience, Neuronal memory allocation

Abstract

N-Cadherin and β-catenin form a transsynaptic adhesion complex required for spine and synapse development. In adulthood, N-cadherin mediates persistent synaptic plasticity, but whether the role of N-cadherin at mature synapses is similar to that at developing synapses is unclear. To address this, we conditionally ablated N-cadherin from excitatory forebrain synapses in mice starting in late postnatal life and examined hippocampal structure and function in adulthood. In the absence of N-cadherin, β-catenin levels were reduced, but numbers of excitatory synapses were unchanged, and there was no impact on number or shape of dendrites or spines. However, the composition of synaptic molecules was altered. Levels of GluA1 and its scaffolding protein PSD95 were diminished and the density of immunolabeled puncta was decreased, without effects on other glutamate receptors and their scaffolding proteins. Additionally, loss of N-cadherin at excitatory synapses triggered increases in the density of markers for inhibitory synapses and decreased severity of hippocampal seizures. Finally, adult mutant mice were profoundly impaired in hippocampal-dependent memory for spatial episodes. These results demonstrate a novel function for the N-cadherin/β-catenin complex in regulating ionotropic receptor composition of excitatory synapses, an appropriate balance of excitatory and inhibitory synaptic proteins and the maintenance of neural circuitry necessary to generate flexible yet persistent cognitive and synaptic function.

Published

2014

2. Synaptic loss and retention of different classic cadherins with LTP-associated synaptic structural remodeling in vivo

Author

Shekhar B. Patil, Deanna L. Benson, George W. Huntley, Oswald Steward, Alice Elste, and Ozlem Bozdagi

Subjects

Male, Synaptic scaling, Protein Stability, Chemistry, Synaptic pharmacology, Cognitive Neuroscience, Long-Term Potentiation, Long-term potentiation, Cadherins, Article, Rats, Rats, Sprague-Dawley, Synaptic fatigue, Synaptic augmentation, Dentate Gyrus, Synapses, Metaplasticity, Synaptic plasticity, Animals, Neuroscience, Synaptic tagging

Abstract

Cadherins are synaptic cell adhesion molecules that contribute to persistently enhanced synaptic strength characteristic of long-term potentiation (LTP). What is relatively unexplored is how synaptic activity of the kind that induces LTP-associated remodeling of synapse structure affects localization of cadherins, particularly in mature animals in vivo, details which could offer insight into how different cadherins contribute to synaptic plasticity. Here, we use a well-described in vivo LTP induction protocol that produces robust synaptic morphological remodeling in dentate gyrus of adult rats in combination with confocal and immunogold electron microscopy to localize cadherin-8 and N-cadherin at remodeled synapses. We find that the density and size of cadherin-8 puncta are significantly diminished in the potentiated middle molecular layer (MML) while concurrently, N-cadherin remains tightly clustered at remodeled synapses. These changes are specific to the potentiated MML, and occur without any change in density or size of synaptophysin puncta. Thus, the loss of cadherin-8 probably represents selective removal from synapses rather than overall loss of synaptic junctions. Together, these findings suggest that activity-regulated loss and retention of different synaptic cadherins could contribute to dual demands of both flexibility and stability in synapse structure that may be important for synaptic morphological remodeling that accompanies long-lasting plasticity.

Published

2010

3. Building and remodeling synapses

Author

Deanna L. Benson and George W. Huntley

Subjects

Neuropil, Synaptic cleft, Cognitive Neuroscience, Cell Adhesion Molecules, Neuronal, Synaptic Membranes, Nerve Tissue Proteins, Neurotransmission, Synaptic Transmission, Article, Synapse, Postsynaptic potential, Metaplasticity, medicine, Animals, Humans, Neuronal Plasticity, Synaptic pharmacology, Chemistry, Serine Endopeptidases, Matrix Metalloproteinases, Extracellular Matrix, medicine.anatomical_structure, Synaptic plasticity, Proteolysis, Neuroscience

Abstract

Synaptic junctions are generated by adhesion proteins that bridge the synaptic cleft to firmly anchor pre- and postsynaptic membranes. Several cell adhesion molecule (CAM) families localize to synapses, but it is not yet completely understood how each synaptic CAM family contributes to synapse formation and/or structure, and whether or how smaller groups of CAMs serve as minimal, functionally cooperative adhesive units upon which structure is based. Synapse structure and function evolve over the course of development, and in mature animals, synapses are composed of a greater number of proteins, surrounded by a stabilizing extracellular matrix, and often contacted by astrocytic processes. Thus, in mature networks undergoing plasticity, persistent changes in synapse strength, morphology, or number must be accompanied by selective and regulated remodeling of the neuropil. Recent work indicates that regulated, extracellular proteolysis may be essential for this, and rather than simply acting permissively to enable synapse plasticity, is more likely playing a proactive role in driving coordinated synaptic structural and functional modifications that underlie persistent changes in network activity.

Published

2010