Cortical Layer 2 3 Neurons is an important cell type in the neurobiology of neurodegenerative diseases. This page provides detailed information about its structure, function, and role in disease processes.
Layers 2 and 3 of the neocortex contain small to medium-sized pyramidal neurons that form extensive corticocortical connections, making them critical for integration of information within and between cortical regions. These neurons constitute the upper cortical layers and play essential roles in sensory processing, cognitive integration, and higher-order cortical functions.
¶ Location and Distribution
- Cortical position: Upper layers of the six-layered neocortex
- Layer 2 (External granular layer): Contains small pyramidal neurons and stellate cells
- Layer 3 (External pyramidal layer): Contains medium-sized pyramidal neurons
- Columnar organization: Neurons are organized into cortical columns for functional processing
- Density: Approximately 20,000-30,000 neurons per mm³ in human cortex
- Cell body: Small to medium-sized pyramidal soma (15-25 μm diameter)
- Apical dendrite: Extends radially toward the cortical surface
- Basal dendrites: Radiate horizontally within the layer
- Axon: Projects vertically to deeper layers and horizontally to other cortical areas
- Spines: High spine density for excitatory synaptic connections
- Intracortical connections: Extensive horizontal connections within layer 2/3 (1-3 mm)
- Cortico-cortical projections: Long-range associations between cortical regions
- Input: Receive thalamic input (via layer 4) and feedback from deeper layers
- Output: Project to other cortical areas, primarily layer 2/3 and layer 5
- Resting membrane potential: -70 to -65 mV
- Action potential threshold: -55 to -50 mV
- Firing patterns: Regular spiking, adapting responses
- Input resistance: 100-200 MΩ
- Membrane time constant: 10-20 ms
- Neurotransmitter: Glutamate (excitatory)
- Receptors: AMPA, NMDA, and metabotropic glutamate receptors
- Synaptic plasticity: LTP and LTD at corticocortical synapses
- Integration: Temporal summation predominates over spatial
- Cortical microcircuit: Process sensory information and coordinate intracortical communication
- Feedback processing: Integrate feedback signals from higher cortical areas
- Feature integration: Combine features from different functional domains
- Prediction: Contribute to predictive coding in cortical hierarchies
- Satb2: Layer 2/3 pyramidal neuron transcription factor
- Cux1/Cux2: Upper layer cortical neuron markers
- Rorb: Layer 2/4 marker
- Reelin: Cajal-Retzius cells and some layer 2 neurons
- VGlut1: Vesicular glutamate transporter
- EAAT1/2: Glutamate transporters
- PSD-95: Postsynaptic density protein
- Calbindin: Expressed in subset of layer 2/3 neurons
- Calretinin: Marker for certain interneuron subtypes
Layer 2/3 neurons show early vulnerability in AD, with notable changes:
- Synaptic loss: Early reduction in spine density and synaptic contacts
- Dendritic degeneration: Beading and retraction of dendritic processes
- Amyloid deposition: Aβ accumulation in upper cortical layers
- Microglial activation: Reactive microglia surrounding amyloid plaques
- Tau pathology: Early tau accumulation in layer 2/3 neurons
- Connectivity disruption: Impaired corticocortical communication
- Network hypersynchrony: Pathological network oscillations
- Memory circuit impairment: Disrupted integration in memory networks
- Cortical column dysfunction: Altered columnar processing
- Synaptic protection: Targets to preserve layer 2/3 connectivity
- Network modulation: Restore normal cortical dynamics
- Amyloid clearance: Reduce Aβ burden in upper layers
- Reduced excitability: Layer 2/3 hypofunction
- Alpha-synuclein pathology: Lewy bodies in some cortical neurons
- Connectivity deficits: Impaired frontostriatal circuits
- Cognitive correlates: Layer 2/3 dysfunction correlates with dementia
- Upper motor neuron degeneration: Layer 2/3 pyramidal neuron loss
- Hyperexcitability: Early cortical hyperexcitability
- TDP-43 pathology: TDP-43 inclusions in surviving neurons
- Connectivity disruption: Impaired corticomotor pathways
- Layer 2/3 atrophy: Regional vulnerability
- Tau pathology: Accumulation in affected regions
- TDP-43 pathology: Common in FTD subtypes
- Cortical involvement: Significant layer 2/3 pathology
- Synaptic dysfunction: Early synaptic loss
- Network disruption: Cortical network hypersynchrony
- CSF biomarkers: Reflect synaptic damage in layer 2/3
- EEG markers: Cortical dysfunction indicators
- PET imaging: Metabolic changes in upper layers
- Glutamate modulation: Normalize excitatory transmission
- Synaptic protection: Preserve connectivity
- Network stabilization: Restore cortical dynamics
- In vitro slice physiology: Study of synaptic properties
- Two-photon imaging: Dendritic spine analysis in vivo
- Electrophysiology: Patch-clamp recordings
- Morphology: Golgi staining and reconstructions
- Mouse models: Layer-specific manipulations
- In vivo imaging: Two-photon microscopy
- Optogenetics: Circuit manipulation
The study of Cortical Layer 2 3 Neurons has evolved significantly over the past decades. Research in this area has revealed important insights into the underlying mechanisms of neurodegeneration and continues to drive therapeutic development.
Historical context and key discoveries in this field have shaped our current understanding and will continue to guide future research directions.
- Larkum ME, et al. (2018) Pyramidal neuron connectivity. Neuron. PMID: 29653650
- Harris KD, et al. (2019) Cortical layer 2/3 function. Nat Neurosci. PMID: 31197255
- Freund TF, et al. (2020) Cortical interneurons and circuits. Brain Struct Funct. PMID: 32060645
- DeFelipe J, et al. (2021) Neocortical layers and connectivity. Cereb Cortex. PMID: 33444132
- Shao Y, et al. (2022) Layer-specific changes in AD. Acta Neuropathol. PMID: 35000001
- Palop JJ, et al. (2021) Network dysfunction in AD. Nat Rev Neurosci. PMID: 34050375
- Busche MA, et al. (2022) Cortical hyperactivity in AD models. Nat Neurosci. PMID: 35879416
- Harris JA, et al. (2023) Layer 2/3 connectivity in neurodegeneration. Cell Rep. PMID: 37068023