4.7 Article

Stimulus feature selectivity in excitatory and inhibitory neurons in primary visual cortex

Journal

JOURNAL OF NEUROSCIENCE
Volume 27, Issue 39, Pages 10333-10344

Publisher

SOC NEUROSCIENCE
DOI: 10.1523/JNEUROSCI.1692-07.2007

Keywords

intracellular; orientation; spatial frequency; synaptic noise; tuning; time constant

Categories

Funding

  1. NEI NIH HHS [R01 EY016430-04] Funding Source: Medline
  2. NIMH NIH HHS [P50 MH064045-10, P50 MH064045] Funding Source: Medline

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Although several lines of evidence suggest that stimulus selectivity in somatosensory and visual cortices is critically dependent on unselective inhibition, particularly in the thalamorecipient layer 4, no comprehensive comparison of the responses of excitatory and inhibitory cells has been conducted. Here, we recorded intracellularly from a large population of regular spiking (RS; presumed excitatory) and fast spiking (FS; presumed inhibitory) cells in layers 2-6 of primary visual cortex. In layer 4, where selectivity for orientation and spatial frequency first emerges, we found no untuned FS cells. Instead, the tuning of the spike output of layer 4 FS cells was significantly but moderately broader than that of RS cells. However, the tuning of the underlying synaptic responses was not different, indicating that the difference in spike-output selectivity resulted from differences in the transformation of synaptic input into firing rate. Layer 4 FS cells exhibited significantly lower input resistance and faster time constants than layer 4 RS cells, leading to larger and faster membrane potential (V-m) fluctuations. FS cell V-m fluctuations were more broadly tuned than those of RS cells and matched spike-output tuning, suggesting that the broader spike tuning of these cells was driven by visually evoked synaptic noise. These differences were not observed outside of layer 4. Thus, cell type-specific differences in stimulus feature selectivity at the first level of cortical sensory processing may arise as a result of distinct biophysical properties that determine the dynamics of synaptic integration.

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