The autism-associated loss of δ-catenin functions disrupts social behaviors

Abstract: δ–catenin is expressed in excitatory synapses and functions as an anchor for the glutamatergic AMPA receptor (AMPAR) GluA2 subunit in the postsynaptic density. The glycine 34 to serine (G34S) mutation in theδ–cateningene is found in autism spectrum disorder (ASD) patients and induces loss of δ–catenin functions at excitatory synapses, which is presumed to underlie ASD pathogenesis in humans. However, how the G34S mutation causes loss of δ–catenin functions to induce ASD remains unclear. Here, using neuroblasto… Show more