It has been demonstrated using single-cell and multiunit electrophysiology in layer III entorhinal cortex and disinhibited hippocampal CA3 slices that the balancing of the up-down activity is characterized by both GABAA and GABAB mechanisms. Here we report novel results obtained using multi-electrode array (60 electrodes) simultaneous recordings from reverberating postnatal neocortical networks containing 19.2 ± 1.4% GABAergic neurons, typical of intact tissue. We observed that in each spontaneous active-state the total number of spikes in identifi ed clusters of excitatory and inhibitory neurons is almost equal, thus suggesting a balanced average activity. Interestingly, in the active-state, the early phase is sustained by only 10% of the total spikes and the fi ring rate follows a sigmoidal regenerative mode up to peak at 35 ms with the number of excitatory spikes greater than inhibitory, therefore indicating an early unbalance. Concentrationresponse pharmacology of up- and down-state lifetimes in clusters of excitatory (n = 1067) and inhibitory (n = 305) cells suggests that, besides the GABAA and GABAB mechanisms, others such as GAT-1-mediated uptake, Ih, INaP and IM ion channel activity, robustly govern both upand down-activity. Some drugs resulted to affect up- and/or down-states with different IC50s, providing evidence that various mechanisms are involved. These results should reinforce not only the role of synchrony in CNS networks, but also the recognized analogies between the Hodgkin-Huxley action potential and the population bursts as basic mechanisms for originating membrane excitability and CNS network synchronization, respectively.

Gullo, F., Mazzetti, S., Maffezzoli, A., Dossi, E., Lecchi, M., Amadeo, A., et al. (2010). Orchestration of presto and largo synchrony in up-down activity of cortical networks. FRONTIERS IN NEURAL CIRCUITS, 4(11) [10.3389/fncir.2010.00011].

Orchestration of presto and largo synchrony in up-down activity of cortical networks

GULLO, FRANCESCA;MAFFEZZOLI, ANDREA;DOSSI, ELENA;LECCHI, MARZIA MARIA;WANKE, ENZO
2010

Abstract

It has been demonstrated using single-cell and multiunit electrophysiology in layer III entorhinal cortex and disinhibited hippocampal CA3 slices that the balancing of the up-down activity is characterized by both GABAA and GABAB mechanisms. Here we report novel results obtained using multi-electrode array (60 electrodes) simultaneous recordings from reverberating postnatal neocortical networks containing 19.2 ± 1.4% GABAergic neurons, typical of intact tissue. We observed that in each spontaneous active-state the total number of spikes in identifi ed clusters of excitatory and inhibitory neurons is almost equal, thus suggesting a balanced average activity. Interestingly, in the active-state, the early phase is sustained by only 10% of the total spikes and the fi ring rate follows a sigmoidal regenerative mode up to peak at 35 ms with the number of excitatory spikes greater than inhibitory, therefore indicating an early unbalance. Concentrationresponse pharmacology of up- and down-state lifetimes in clusters of excitatory (n = 1067) and inhibitory (n = 305) cells suggests that, besides the GABAA and GABAB mechanisms, others such as GAT-1-mediated uptake, Ih, INaP and IM ion channel activity, robustly govern both upand down-activity. Some drugs resulted to affect up- and/or down-states with different IC50s, providing evidence that various mechanisms are involved. These results should reinforce not only the role of synchrony in CNS networks, but also the recognized analogies between the Hodgkin-Huxley action potential and the population bursts as basic mechanisms for originating membrane excitability and CNS network synchronization, respectively.
Articolo in rivista - Articolo scientifico
Bursts; GABA; I; h; channels; I; m; channels; I; NaP; channels; MEA recording; Synchrony;
English
2010
4
11
9
open
Gullo, F., Mazzetti, S., Maffezzoli, A., Dossi, E., Lecchi, M., Amadeo, A., et al. (2010). Orchestration of presto and largo synchrony in up-down activity of cortical networks. FRONTIERS IN NEURAL CIRCUITS, 4(11) [10.3389/fncir.2010.00011].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10281/10651
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