The basic requirement for direction selectivity is a nonlinear interaction between two different inputs in space-time. In some models, the interaction is hypothesized to occur between excitation and inhibition of the shunting type in the neuron's dendritic tree. How can the required spatial specificity be acquired in an unsupervised manner? We here propose an activity-based, local learning model that can account for direction selectivity in visual cortex based on such a local veto operation and that depends on synaptically induced changes in intracellular calcium concentration. Our biophysical simulations suggest that a model cell with our learning algorithm can develop direction selectivity organically after unsupervised training. The learning rule is also applicable to a neuron with multiple-direction-selective subunits and to a pair of cells with opposite-direction selectivities and is stable under different starting conditions, delays, and velocities.

Reverse-phi motion is the illusory reversal of perceived direction of movement when the stimulus contrast is reversed in successive frames. Livingstone, Tsao, and Conway (2000) showed that direction-selective cells in striate cortex of the alert macaque monkey showed reversed excitatory and inhibitory regions when two different contrast bars were flashed sequentially during a two-bar interaction analysis. While correlation or motion energy models predict the reverse-phi response, it is unclear how neurons can accomplish this. We carried out detailed biophysical simulations of a direction-selective cell model implementing a synaptic shunting scheme. Our results suggest that a simple synaptic-veto mechanism with strong direction selectivity for normal motion cannot account for the observed reverse-phi motion effect. Given the nature of reverse-phi motion, a direct interaction between the ON and OFF pathway, missing in the original shunting-inhibition model, it is essential to account for the reversal of response. We here propose a double synaptic-veto mechanism in which ON excitatory synapses are gated by both delayed ON inhibition at their null side and delayed OFF inhibition at their preferred side. The converse applies to OFF excitatory synapses. Mapping this scheme onto the dendrites of a direction-selective neuron permits the model to respond best to normal motion in its preferred direction and to reverse-phi motion in its null direction. Two-bar interaction maps showed reversed excitation and inhibition regions when two different contrast bars are presented.