SOX2 O-GlcNAcylation alters its protein-protein interactions and genomic occupancy to modulate gene expression in pluripotent cells.

SOX2 is a transcription factor that is central to the identity of many cell types, including embryonic stem cells (ESCs), neural stem cells and pancreatic precursors. In each cell type SOX2 directs expression of a set of genes unique to that cell type. One mechanism by which the same transcription factor can mediate very different outputs is regulation by post-translational modifications (PTMs) - chemical changes to the protein that affect its ability to interact with other proteins or bind to DNA. We characterized the PTM profile of SOX2 in ESCs and differentiating ESCs and find that SOX2 PTMs are developmentally regulated. In ESCs SOX2 is subject to a poorly understood PTM, the addition of an O-linked N-acetylglucosamine sugar, which is a nutrient responsive modification. Mutational analysis of SOX2 that cannot be modified showed that this PTM regulates the ability of SOX2 to interact with protein partners and controls which regions of the genetic code SOX2 occupies. These studies link a nutrient sensing PTM to pluripotency via regulation of a key pluripotency transcription factor.