Abstract

Gamma-band oscillations arise from the interplay between neural excitation (E) and inhibition (I) and may provide a non-invasive window into the state of cortical circuitry. A bell-shaped modulation of gamma response power by increasing the intensity of sensory input was observed in animals and is thought to reflect neural gain control. Here we sought to find a similar input-output relationship in humans with MEG via modulating the intensity of a visual stimulation by changing the velocity/temporal-frequency of visual motion. In the first experiment, adult participants observed static and moving gratings. The frequency of the MEG gamma response monotonically increased with motion velocity whereas power followed a bell-shape. In the second experiment, on a large group of children and adults, we found that despite drastic developmental changes in frequency and power of gamma oscillations, the relative suppression at high motion velocities was scaled to the same range of values across the life-span. In light of animal and modeling studies, the modulation of gamma power and frequency at high stimulation intensities characterizes the capacity of inhibitory neurons to counterbalance increasing excitation in visual networks. Gamma suppression may thus provide a non-invasive measure of inhibitory-based gain control in the healthy and diseased brain.

Highlights

  • May provide a non-invasive window into the state of cortical circuitry

  • This contradicts the idea that the peak frequency of gamma response

  • We found that increasing the velocity of visual motion from 0 to 6°/s resulted in an approximately linear increase in frequency and clearly nonlinear changes in power of sustained gamma oscillations in MEG

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Summary

Introduction

May provide a non-invasive window into the state of cortical circuitry. A bell-shaped modulation of gamma response power by increasing the intensity of sensory input was observed in animals and is thought to reflect neural gain control. We predicted that modulating excitatory drive to the cortex (by increasing the velocity/temporal frequency of visual motion) would result in a monotonic increase of MEG gamma peak frequency and concurrent bell-shaped change in gamma power. All participants showed highly reliable sustained gamma response to the stimuli, with a monotonic increase of gamma oscillation frequency as a function of visual motion velocity.

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