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The interplay between homeostatic synaptic scaling and homeostatic structural plasticity maintains the robust firing rate of neural networks
by
Diaz-Pier, Sandra
, Lenz, Maximilian
, Lu, Han
, Vlachos, Andreas
in
Animals
/ Dendritic spines
/ Entorhinal Cortex - physiology
/ Female
/ Firing rate
/ Hebbian plasticity
/ Hippocampus
/ Hippocampus - physiology
/ Homeostasis
/ Homeostatic plasticity
/ Information processing
/ Male
/ Mice
/ Nerve Net - physiology
/ Neural networks
/ Neuronal Plasticity - physiology
/ Neurons
/ Neurons - physiology
/ Neuroplasticity
/ Neurotransmission
/ organotypic slice cultures
/ Quinoxaline
/ Receptor density
/ Receptors, AMPA - antagonists & inhibitors
/ Receptors, AMPA - metabolism
/ Scaling
/ spiking neural networks
/ structural plasticity
/ Synapses
/ Synapses - physiology
/ Synaptic plasticity
/ synaptic scaling
/ Synaptic strength
/ Synaptogenesis
/ α-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid
/ α-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid receptors
2025
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The interplay between homeostatic synaptic scaling and homeostatic structural plasticity maintains the robust firing rate of neural networks
by
Diaz-Pier, Sandra
, Lenz, Maximilian
, Lu, Han
, Vlachos, Andreas
in
Animals
/ Dendritic spines
/ Entorhinal Cortex - physiology
/ Female
/ Firing rate
/ Hebbian plasticity
/ Hippocampus
/ Hippocampus - physiology
/ Homeostasis
/ Homeostatic plasticity
/ Information processing
/ Male
/ Mice
/ Nerve Net - physiology
/ Neural networks
/ Neuronal Plasticity - physiology
/ Neurons
/ Neurons - physiology
/ Neuroplasticity
/ Neurotransmission
/ organotypic slice cultures
/ Quinoxaline
/ Receptor density
/ Receptors, AMPA - antagonists & inhibitors
/ Receptors, AMPA - metabolism
/ Scaling
/ spiking neural networks
/ structural plasticity
/ Synapses
/ Synapses - physiology
/ Synaptic plasticity
/ synaptic scaling
/ Synaptic strength
/ Synaptogenesis
/ α-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid
/ α-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid receptors
2025
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The interplay between homeostatic synaptic scaling and homeostatic structural plasticity maintains the robust firing rate of neural networks
by
Diaz-Pier, Sandra
, Lenz, Maximilian
, Lu, Han
, Vlachos, Andreas
in
Animals
/ Dendritic spines
/ Entorhinal Cortex - physiology
/ Female
/ Firing rate
/ Hebbian plasticity
/ Hippocampus
/ Hippocampus - physiology
/ Homeostasis
/ Homeostatic plasticity
/ Information processing
/ Male
/ Mice
/ Nerve Net - physiology
/ Neural networks
/ Neuronal Plasticity - physiology
/ Neurons
/ Neurons - physiology
/ Neuroplasticity
/ Neurotransmission
/ organotypic slice cultures
/ Quinoxaline
/ Receptor density
/ Receptors, AMPA - antagonists & inhibitors
/ Receptors, AMPA - metabolism
/ Scaling
/ spiking neural networks
/ structural plasticity
/ Synapses
/ Synapses - physiology
/ Synaptic plasticity
/ synaptic scaling
/ Synaptic strength
/ Synaptogenesis
/ α-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid
/ α-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid receptors
2025
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The interplay between homeostatic synaptic scaling and homeostatic structural plasticity maintains the robust firing rate of neural networks
Journal Article
The interplay between homeostatic synaptic scaling and homeostatic structural plasticity maintains the robust firing rate of neural networks
2025
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Overview
Critical network states and neural plasticity enable adaptive behavior in dynamic environments, supporting efficient information processing and experience-dependent learning. Synaptic-weight-based Hebbian plasticity and homeostatic synaptic scaling are key mechanisms that enable memory while stabilizing network dynamics. However, the role of structural plasticity as a homeostatic mechanism remains less consistently reported, particularly under activity inhibition, leading to an incomplete understanding of its functional impact. In this study, we combined live-cell microscopy of eGFP-labeled neurons in mouse organotypic entorhinal-hippocampal tissue cultures (Thy1-eGFP mice of both sexes) with computational modeling to investigate how synapse-number-based structural plasticity responds to activity perturbations and interacts with homeostatic synaptic scaling. Tracking individual dendritic segments, we found that inhibiting excitatory neurotransmission does not monotonically regulate dendritic spine density. Specifically, inhibition of AMPA receptors with 200 nM 2,3-dioxo-6-nitro-7-sulfamoyl-benzo[f]quinoxaline (NBQX) increased spine density, whereas complete AMPA receptor blockade with 50 μM NBQX reduced it. Motivated by these findings, we developed network simulations incorporating a biphasic structural plasticity rule governing activity-dependent synapse formation. These simulations showed that the biphasic rule maintains neural activity homeostasis under stimulation and permits either synapse formation or synapse loss depending on the degree of activity deprivation. Homeostatic synaptic scaling further modulated recurrent connectivity, network activity, and structural plasticity outcomes. It reduced stimulation-triggered synapse loss by downscaling synaptic weights and rescued silencing-induced synapse loss by upscaling recurrent input, thus reactivating silent neurons. The interaction between these mechanisms provides a mechanistic explanation for divergent findings in the literature. In summary, homeostatic synaptic scaling and homeostatic structural plasticity dynamically compete and compensate for each other, ensuring efficient and robust control of firing rate homeostasis.
Publisher
eLife Sciences Publications Ltd
Subject
/ Entorhinal Cortex - physiology
/ Female
/ Male
/ Mice
/ Neuronal Plasticity - physiology
/ Neurons
/ Receptors, AMPA - antagonists & inhibitors
/ Receptors, AMPA - metabolism
/ Scaling
/ Synapses
/ α-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid
/ α-Amino-3-hydroxy-5-methyl-4-isoxazole propionic acid receptors
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