ORDB: Neuron - Dentate gyrus granule GLU cell

Neuron

Data

Name

Dentate gyrus granule GLU cell

Picture

Canonical Form Type

Canonical form 2 Show Other

Picture from

Lomo, Patterns of activation in a monosynaptic cortical pathway: The perforant path input to the dentate area of the hippcampal formation, Experimental Brain Research, 1971 12:46-63.

Organism

Vertebrates Show Other

Neuron category

principal Show Other

Neuron type

Granular Show Other

cell rotation

Coordinates(2D)

399,122

Description

The principal neuron of the fascia dentata of the hippocampal region. It forms a single layer of cell bodies. Each cell has a dendritic tree that extends toward the surface. The branches are covered with dendritic spines. The input is carried by axons which arise in the nearby entorinal cortex and "perforate" the intervening cortex to make excitatory glutamatergic synapses onto the spines. The output is carried in an axon which becomes a mossy fiber as it arrives in CA3 and CA2 of the hippocampus to make glutamatergic synapes onto the spinous excrecenses of hippocampal pyramidal cells in those regions.

Electrophysiological properties

NeuroLex

Layer

Hodology

Molecular Marker

Neuronal Receptors (23)

SN	Property present	CF-Compartment	Receptor	Connect Note	Publication facts
1	Yes	Distal equivalent dendrite	NMDA	Perforant path terminals
2	Yes	Distal equivalent dendrite	AMPA	Perforant path terminals
3	Yes	Distal equivalent dendrite	mGluR	Perforant path terminals
4	Yes	Distal equivalent dendrite	GabaA	Hilar spiny interneuron terminals
5	Yes	Distal equivalent dendrite	GabaB	Hilar spiny interneuron terminals
6	Yes	Middle equivalent dendrite	AMPA	Perforant path terminals
7	Yes	Middle equivalent dendrite	mGluR	Perforant path terminals
8	Yes	Middle equivalent dendrite	GabaA	Hilar spiny and aspiny interneuron terminals
9	Yes	Middle equivalent dendrite	NMDA	Perforant path terminals
10	Yes	Middle equivalent dendrite	GabaB	Hilar spiny and aspiny interneuron terminals
11	Yes	Proximal equivalent dendrite	NMDA	Hilar mossy cell collaterals and commissural cell terminals
12	Yes	Proximal equivalent dendrite	GabaB	Hilar aspiny interneuron terminals
13	Yes	Proximal equivalent dendrite	mGluR	Hilar mossy cell collaterals and commissural cell terminals
14	Yes	Proximal equivalent dendrite	AMPA	Hilar mossy cell collaterals and commissural cell terminals
15	Yes	Proximal equivalent dendrite	GabaA	Hilar aspiny interneuron terminals
16	Yes	Axon hillock	GabaA	Chandelier cell terminals
17	Yes	Axon hillock	GabaB	Chandelier cell terminals
18	Yes	Soma	GabaA	Basket cell terminals	Whole cell and perforated patch recordings in slices showed bicuculline-dependent and ?independent GABA currents from juvenile rats, suggesting two types of GABAergic inputs. The bicuculline-independent component was present only at the earliest stages of maturation, had a later peak, slower time course of decay, and marked outward rectification. A trophic or signaling role rather than primarily inhibitory was suggested for this current
19	Yes	Soma	AMPA		NMDA and AMPA conductances properties were studied using patch-clamp recordings in morphologically identified cells in slices prepared from surgically removed medial temporal lobe specimens of epileptic patients (14 specimens from 14 patients
20	Yes	Soma	NMDA		NMDA and AMPA conductances properties were studied using patch-clamp recordings in morphologically identified cells in slices prepared from surgically removed medial temporal lobe specimens of epileptic patients (14 specimens from 14 patients). The wide range of changes in the slope conductance of the NMDA EPSCs suggests that the NMDA-receptor-mediated conductance could be altered in human epileptic DGCs
21	Yes	Soma	GabaB	Basket cell terminals
22	Yes	Soma	Nicotinic
23	Yes	Axon terminal	Kainate		It has been shown that activation of these receptors could facilitate transmitter release. Their activation is very fast (<10 ms) and lasts for seconds, and could contribute to the short-term plasticity characteristics of mossy fiber synapses

Neuronal Currents (23)

SN	Property present	CF-Compartment	Current	Publication facts
1	Yes	Distal equivalent dendrite	I Na,t
2	Yes	Distal equivalent dendrite	I A
3	Yes	Distal equivalent dendrite	I L high threshold
4	Yes	Distal equivalent dendrite	I Na,p	low density
5	Yes	Middle equivalent dendrite	I L high threshold
6	Yes	Middle equivalent dendrite	I Na,p	low density
7	Yes	Proximal equivalent dendrite	I L high threshold
8	Yes	Proximal equivalent dendrite	I Na,p
9	Yes	Axon hillock	I K
10	Yes	Axon hillock	I Na,t
11	Yes	Axon hillock	I K,Ca
12	Yes	Axon terminal	I N
13	Yes	Soma	I K,Ca	Voltage-clamp analysis suggested that IAHP in DG neurones is generated by about 1200 channels, and that about 60% are open at the peak of a maximal IAHP
14	Yes	Soma	I L high threshold	Patch-clamp recordings from human cells showed N-type, L-type and T-type currents that had similar pharmacological and kinetic characteristics as in control rats. The current density was significantly larger in human and in the kainate model compared to cells isolated from adult control rats
15	Yes	Soma	I N	Patch-clamp recordings from human cells showed N-type, L-type and T-type currents that had similar pharmacological and kinetic characteristics as in control rats. The current density was significantly larger in human and in the kainate model compared to cells isolated from adult control rats
16	Yes	Soma	I T low threshold	Patch-clamp recordings from human cells showed N-type, L-type and T-type currents that had similar pharmacological and kinetic characteristics as in control rats. The current density was significantly larger in human and in the kainate model compared to cells isolated from adult control rats
17	Yes	Soma	I A	The properties of outward currents were investigated with patch-clamp in acutely isolated cells at various postnatal ages and at adulthood (2-3 mo). Kinetic analysis and pharmacological properties showed that IK and IA were present in these cells. IA and IK remained stable with respect to kinetic properties during ontogenesis, but the relative contribution and pharmacological properties varied with age. IA dominated in P5-7 cells whereas IK was prominent in most older cells
18		Soma	I h	Patch-pipette recordings found no evidence for a ?sag? in hyperpolarizing responses, suggesting that this current is not present in these neurons
19	Yes	Middle equivalent dendrite	I Na,t	Indirect experimental evidence for dendritic Na channels was suggested by laminar filed potential studies
20	Yes	Proximal equivalent dendrite	I Na,t	Indirect experimental evidence for dendritic Na channels was suggested by laminar filed potential studies
21	Yes	Soma	I Na,t	The kinetic properties of this current were studied using the whole-cell voltage-clamp method in acutely isolated cells. No significant differences were found after induction of status epilepticus
22	Yes	Soma	I K	The properties of outward currents were investigated with patch-clamp in acutely isolated rat DGCs at various postnatal ages and at adulthood (2-3 mo). Kinetic analysis and pharmacological properties showed that IK and IA were present in these cells. IA and IK remained stable with respect to kinetic properties during ontogenesis, but the relative contribution and pharmacological properties varied with age. IA dominated in P5-7 cells whereas IK was prominent in most older cells
23	Yes	Axon terminal	I L high threshold	Transients and kinetics for these channels were studied using whole-cell patch clamp recordings

Neuronal Transmitters (6)

SN	Property present	CF-Compartment	transmitter	Connect Note	Publication facts
1	Yes	Axon terminal	Zn2+	CA3 pyramidal neuron proximal dendrites, mossy cell proximal dendrites, and basket cell basal dendrites
2	Yes	Axon terminal	Glutamate	CA3 pyramidal neuron proximal dendrites, mossy cell proximal dendrites, and basket cell basal dendrites
3	Yes	Axon fiber	Glutamate	To presynaptic kainate receptors in the CA3 region of the hippocampus	Glutamate - kainate receptor (glur6)In mouse hippocampal slices, bath application of kainate caused presynaptic reduction in epscs at mossy fiber synapses on CA3 pyramidal cells in glur6 knockouts but not in glur5 knockouts.
4	Yes	Middle equivalent dendrite	Dynorphin	Perforant path terminals
5	Yes	Distal equivalent dendrite	Dynorphin	Perforant path terminals
6	Yes	Axon terminal	Dynorphin	CA3 pyramidal neuron proximal dendrites, mossy cell proximal dendrites, and basket cell basal dendrites

Other categories referring to Dentate gyrus granule GLU cell

Pathological mechanism.Neuron (1)

2 Objects Relationship (edge).Object Two (target) (1)

Neural compartmental intracell.Neuron (1)

Cell Type.NeuronDB Neuron (1)

Neuronal Structure.Neurons (1)

ICG channel details.ICG ModelDB cell (3)

Revisions:	13
Last Time:	12/18/2015 11:13:46 AM
Reviewer:	System Administrator
Owner:	System Administrator