4.8 Article

Intrinsic excitability mechanisms of neuronal ensemble formation

Journal

ELIFE
Volume 11, Issue -, Pages -

Publisher

eLIFE SCIENCES PUBL LTD
DOI: 10.7554/eLife.77470

Keywords

ensembles; intrinsic excitability; optogenetics; visual cortex; Hebbian plasticity; synaptic connection; Mouse

Categories

Funding

  1. National Council of Science and Technology from Mexico (CONACYT) [R01EY011787, R01MH115900]

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Neuronal ensembles are coactive groups of cortical neurons that play a role in perception and behavior. In this study, we replicated an in vivo optogenetic protocol in brain slices to investigate the mechanisms involved in ensemble formation. We found that coactivated neurons showed increased correlated activity and biphasic changes in presynaptic plasticity. Furthermore, stimulation induced significant increases in spontaneous EPSPs and neuronal excitability.
Neuronal ensembles are coactive groups of cortical neurons, found in spontaneous and evoked activity, that can mediate perception and behavior. To understand the mechanisms that lead to the formation of ensembles, we co-activated layer 2/3 pyramidal neurons in brain slices from mouse visual cortex, in animals of both sexes, replicating in vitro an optogenetic protocol to generate ensembles in vivo. Using whole-cell and perforated patch-clamp pair recordings we found that, after optogenetic or electrical stimulation, coactivated neurons increased their correlated activity, a hallmark of ensemble formation. Coactivated neurons showed small biphasic changes in presynaptic plasticity, with an initial depression followed by a potentiation after a recovery period. Optogenetic and electrical stimulation also induced significant increases in frequency and amplitude of spontaneous EPSPs, even after single-cell stimulation. In addition, we observed unexpected strong and persistent increases in neuronal excitability after stimulation, with increases in membrane resistance and reductions in spike threshold. A pharmacological agent that blocks changes in membrane resistance reverted this effect. These significant increases in excitability can explain the observed biphasic synaptic plasticity. We conclude that cell-intrinsic changes in excitability are involved in the formation of neuronal ensembles. We propose an 'iceberg' model, by which increased neuronal excitability makes subthreshold connections suprathreshold, enhancing the effect of already existing synapses, and generating a new neuronal ensemble.

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