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Driving fast-spiking cells induces gamma rhythm and controls sensory responses.


ABSTRACT: Cortical gamma oscillations (20-80 Hz) predict increases in focused attention, and failure in gamma regulation is a hallmark of neurological and psychiatric disease. Current theory predicts that gamma oscillations are generated by synchronous activity of fast-spiking inhibitory interneurons, with the resulting rhythmic inhibition producing neural ensemble synchrony by generating a narrow window for effective excitation. We causally tested these hypotheses in barrel cortex in vivo by targeting optogenetic manipulation selectively to fast-spiking interneurons. Here we show that light-driven activation of fast-spiking interneurons at varied frequencies (8-200 Hz) selectively amplifies gamma oscillations. In contrast, pyramidal neuron activation amplifies only lower frequency oscillations, a cell-type-specific double dissociation. We found that the timing of a sensory input relative to a gamma cycle determined the amplitude and precision of evoked responses. Our data directly support the fast-spiking-gamma hypothesis and provide the first causal evidence that distinct network activity states can be induced in vivo by cell-type-specific activation.

SUBMITTER: Cardin JA 

PROVIDER: S-EPMC3655711 | biostudies-literature | 2009 Jun

REPOSITORIES: biostudies-literature

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Driving fast-spiking cells induces gamma rhythm and controls sensory responses.

Cardin Jessica A JA   Carlén Marie M   Meletis Konstantinos K   Knoblich Ulf U   Zhang Feng F   Deisseroth Karl K   Tsai Li-Huei LH   Moore Christopher I CI  

Nature 20090426 7247


Cortical gamma oscillations (20-80 Hz) predict increases in focused attention, and failure in gamma regulation is a hallmark of neurological and psychiatric disease. Current theory predicts that gamma oscillations are generated by synchronous activity of fast-spiking inhibitory interneurons, with the resulting rhythmic inhibition producing neural ensemble synchrony by generating a narrow window for effective excitation. We causally tested these hypotheses in barrel cortex in vivo by targeting op  ...[more]

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