Selective disruption of synaptic BMP signaling by a Smad mutation adjacent to the highly conserved H2 helix

Abstract: Bone morphogenetic proteins (BMPs) shape normal development and function via canonical and non-canonical signaling pathways. When activating the canonical pathway, BMPs initiate signaling by binding to transmembrane receptors that phosphorylate pathway effectors, the Smad proteins, inducing their translocation into the nucleus and thus regulation of target genes. Phosphorylated Smads also accumulate at cellular junctions, but this noncanonical signaling modality remains less defined. We have recently reported … Show more