The human cell in health and disease

In commemoration of 100 years since the discovery of glucagon, we review current knowledge about the human a cell. Alpha cells make up 30-40% of human islet endocrine cells and play a major role in regulating whole-body glucose homeostasis, largely through the direct actions of their main secretory product - glucagon - on peripheral organs. Additionally, glucagon and other secretory products of a cells, namely acetylcholine, glutamate, and glucagon-like peptide-1, have been shown to play an indirect role in the modulation of glucose homeostasis through autocrine and paracrine interactions within the islet. Studies of glucagon's role as a counterregulatory hormone have revealed additional important functions of the a cell, including the regulation of multiple aspects of energy metabolism outside that of glucose. At the molecular level, human a cells are defined by the expression of conserved islet-enriched transcription factors and various enriched signature genes, many of which have currently unknown cellular functions. Despite these common threads, notable heterogeneity exists amongst human a cell gene expression and function. Even greater differences are noted at the inter-species level, underscoring the importance of further study of a cell physiology in the human context. Finally, studies on a cell morphology and function in type 1 and type 2 diabetes, as well as other forms of metabolic stress, reveal a key contribution of a cell dysfunction to dysregulated glucose homeostasis in disease pathogenesis, making targeting the a cell an important focus for improving treatment.