Litcius/Paper detail

Not the second fiddle: α cell development, identity, and function in health and diabetes

Elliott P. Brooks, Lori Sussel

2023Journal of Endocrinology14 citationsDOIOpen Access PDF

Abstract

Historic and emerging studies provide evidence for the deterioration of pancreatic α cell function and identity in diabetes mellitus. Increased access to human tissue and the availability of more sophisticated molecular technologies have identified key insights into how α cell function and identity are preserved in healthy conditions and how they become dysfunctional in response to stress. These studies have revealed evidence of impaired glucagon secretion, shifts in α cell electrophysiology, changes in α cell mass, dysregulation of α cell transcription, and α-to-β cell conversion prior to and during diabetes. In this review, we outline the current state of research on α cell identity in health and disease. Evidence in model organisms and humans suggests that in addition to β cell dysfunction, diabetes is associated with a fundamental dysregulation of α cell identity. Importantly, epigenetic studies have revealed that α cells retain more poised and open chromatin at key cell-specific and diabetes-dysregulated genes, supporting the model that the inherent epigenetic plasticity of α cells makes them susceptible to the transcriptional changes that potentiate the loss of identity and function seen in diabetes. Thus, additional research into the maintenance of α cell identity and function is critical to fully understanding diabetes. Furthermore, these studies suggest α cells could represent an alternative source of new β cells for diabetes treatment.

Topics & Concepts

Diabetes mellitusEpigeneticsBiologyCellChromatinBioinformaticsNeuroscienceMedicineCell biologyEndocrinologyGeneticsGenePancreatic function and diabetesDiabetes Management and ResearchDiabetes and associated disorders